For other uses, see Ethanol (disambiguation).
Ethanol |
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Identifiers |
CAS number |
64-17-5 Y |
PubChem |
702 |
ChemSpider |
682 Y |
Jmol-3D images |
Image 1 |
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-
InChI=1S/C2H6O/c1-2-3/h3H,2H2,1H3 Y
Key: LFQSCWFLJHTTHZ-UHFFFAOYSA-N Y
InChI=1/C2H6O/c1-2-3/h3H,2H2,1H3
Key: LFQSCWFLJHTTHZ-UHFFFAOYAB
|
Properties |
Molecular formula |
C2H6O |
Molar mass |
46.07 g mol−1 |
Density |
0.789 g/cm3 (at 25°C) |
Melting point |
−114 °C (−173 °F; 159 K) |
Boiling point |
78.37 °C (173.07 °F; 351.52 K) |
Acidity (pKa) |
15.9 (H2O), 29.8 (DMSO)[2][3] |
Hazards[5] |
MSDS |
External MSDS |
R-phrases |
R11 |
S-phrases |
(S2), S7, S16 |
Flash point |
16 °C (61 °F; 289 K) |
Autoignition temperature |
365 °C (689 °F; 638 K) |
LD50 |
7060 mg/kg (oral, rat)[4] |
Related compounds |
Related compounds |
Methanol
Ethane |
Supplementary data page |
Structure and
properties |
n, εr, etc. |
Thermodynamic
data |
Phase behaviour
Solid, liquid, gas |
Spectral data |
UV, IR, NMR, MS |
Except where noted otherwise, data are given for materials in their standard state (at 25 °C (77 °F), 100 kPa) |
N (verify) (what is: Y/N?) |
Infobox references |
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Commonly referred to simply as alcohol or spirits, ethanol // is also called ethyl alcohol, and drinking alcohol. It is the principal type of alcohol found in alcoholic beverages, produced by the fermentation of sugars by yeasts. It is a neurotoxic[6][7] psychoactive drug and one of the oldest recreational drugs used by humans. It can cause alcohol intoxication when consumed in sufficient quantity. Ethanol is used as a solvent, an antiseptic, a fuel and the active fluid in modern (post-mercury) thermometers. It is a volatile, flammable, colorless liquid with a strong chemical odor. Its structural formula CH
3CH
2OH, is often abbreviated as C
2H
5OH, C
2H
6O or EtOH.
Contents
- 1 Etymology
- 2 Chemical formula
- 3 Natural occurrence
- 4 Pharmacology
- 4.1 Activity profile
- 4.2 Properties
- 4.3 Short-term
- 4.3.1 Effects on the central nervous system
- 4.3.2 Effects on metabolism
- 4.3.3 Drug interactions
- 4.3.4 Alcohol and digestion
- 4.3.5 Alcohol and gastrointestinal diseases
- 4.3.6 Magnitude of effects
- 4.4 Long-term
- 4.4.1 Birth defects
- 4.4.2 Cancer
- 4.4.3 Other effects
- 5 History
- 6 Properties
- 6.1 Physical properties
- 6.2 Solvent properties
- 6.3 Flammability
- 7 Production
- 7.1 Ethylene hydration
- 7.2 Fermentation
- 7.2.1 Cellulose
- 7.2.2 Hydrocarbon
- 7.3 Testing
- 8 Research
- 9 Purification
- 9.1 Distillation
- 9.2 Molecular sieves and desiccants
- 9.3 Membranes and reverse osmosis
- 9.4 Other techniques
- 10 Grades of ethanol
- 10.1 Denatured alcohol
- 10.2 Absolute alcohol
- 10.3 Rectified spirits
- 11 Reactions
- 11.1 Ester formation
- 11.2 Dehydration
- 11.3 Combustion
- 11.4 Acid-base chemistry
- 11.5 Halogenation
- 11.6 Oxidation
- 12 Other uses
- 12.1 Motor fuel
- 12.2 Household heating
- 12.3 Feedstock
- 12.4 Antiseptic
- 12.5 Solvent
- 13 Charts
- 14 History
- 15 See also
- 16 References
- 17 Further reading
- 18 External links
Etymology
Ethanol is the systematic name defined by the International Union of Pure and Applied Chemistry (IUPAC) for a molecule with two carbon atoms (prefix "eth-"), having a single bond between them (suffix "-ane"), and an attached functional group-OH group (suffix "-ol").[1]
The prefix ethyl was coined in 1834 by the German chemist Justus Liebig.[8] Ethyl is a contraction of the French word ether (any substance that evaporated or sublimated readily at room temperature) and the Greek word ύλη (hyle, substance).[9]
The name ethanol was coined as a result of a resolution that was adopted at the International Conference on Chemical Nomenclature that was held in April 1892 in Geneva, Switzerland.[10]
The term "alcohol" now refers to a wider class of substances in chemistry nomenclature, but in common parlance it remains the name of ethanol. Ultimately a medieval loan from Arabic al-kuḥl,[11] use of alcohol in this sense is modern, introduced in the mid 18th century. Before that time, Middle Latin alcohol referred to "powdered ore of antimony; powdered cosmetic", by the later 17th century "any sublimated substance; distilled spirit" use for "the spirit of wine" (shortened from a full expression alcohol of wine) recorded 1753. The systematic use in chemistry dates to 1850.
Chemical formula
Ethanol is a 2-carbon alcohol. Its molecular formula is CH3CH2OH. An alternative notation is CH3–CH2–OH, which indicates that the carbon of a methyl group (CH3–) is attached to the carbon of a methylene group (–CH2–), which is attached to the oxygen of a hydroxyl group (–OH). It is a constitutional isomer of dimethyl ether. Ethanol is sometimes abbreviated as EtOH, using the common organic chemistry notation of representing the ethyl group (C2H5) with Et.
Natural occurrence
Ethanol is a byproduct of the metabolic process of yeast. As such, ethanol will be present in any yeast habitat. Ethanol can commonly be found in overripe fruit.[12] Ethanol produced by symbiotic yeast can be found in Bertam Palm blossoms. Although some animal species such as the Pentailed Treeshrew exhibit ethanol-seeking behaviors, most show no interest or avoidance of food sources containing ethanol.[13] Ethanol is also produced during the germination of many plants as a result of natural anerobiosis.[14] Ethanol has been detected in outer space, forming an icy coating around dust grains in interstellar clouds.[15] Minute quantity amounts (244 ppb) of endogenous ethanol and acetaldehyde were found in the exhaled breath of healthy volunteers.[16] Auto-brewery syndrome, also known as gut fermentation syndrome, is a rare medical condition in which intoxicating quantities of alcohol are produced through endogenous fermentation within the digestive system.[17][18]
Pharmacology
Activity profile
Ethanol is known to possess the following direct pharmacodynamic actions (most important actions are bolded):[19]
Some of its actions on ligand-gated ion channels, specifically the nACh receptors and the glycine receptor, are dose-dependent, with potentiation or inhibition occurring dependent on ethanol concentration. This is because ethanol's effects on these channels are a summation of positive and negative allosteric modulatory actions.[19]
Properties
The removal of ethanol from the human body, through oxidation by alcohol dehydrogenase in the liver, is limited. Hence, the removal of a large concentration of alcohol from blood may follow zero-order kinetics. This means that alcohol leaves the body at a constant rate, rather than having an elimination half-life.[23]
The rate-limiting steps for one substance may be in common with other substances. As a result, the blood alcohol concentration can be used to modify the rate of metabolism of methanol and ethylene glycol. Methanol itself is not highly toxic, but its metabolites formaldehyde and formic acid are; therefore, to reduce the rate of production and concentration of these harmful metabolites, ethanol can be ingested.[24] Ethylene glycol poisoning can be treated in the same way.
Pure ethanol will irritate the skin and eyes.[25] Nausea, vomiting and intoxication are symptoms of ingestion. Long-term use by ingestion can result in serious liver damage.[26] Atmospheric concentrations above one in a thousand are above the European Union Occupational exposure limits.[26]
Short-term
Main article: Short-term effects of alcohol
BAC (g/L) |
BAC
(% v/v) |
Symptoms[27] |
0.5 |
0.05% |
Euphoria, talkativeness, relaxation |
1 |
0.1 % |
Central nervous system depression, nausea, possible vomiting, impaired motor and sensory function, impaired cognition |
>1.4 |
>0.14% |
Decreased blood flow to brain |
3 |
0.3% |
Stupefaction, possible unconsciousness |
4 |
0.4% |
Possible death |
>5.5 |
>0.55% |
Death |
Effects on the central nervous system
Ethanol is a central nervous system depressant and has significant psychoactive effects in sublethal doses; for specifics, see "Effects of alcohol on the body by dose". Based on its abilities to change the human consciousness, ethanol is considered a psychoactive drug.[28] Death from ethanol consumption is possible when blood alcohol level reaches 0.4%. A blood level of 0.5% or more is commonly fatal. Levels of even less than 0.1% can cause intoxication, with unconsciousness often occurring at 0.3–0.4%.[29]
The amount of ethanol in the body is typically quantified by blood alcohol content (BAC), which is here taken as weight of ethanol per unit volume of blood. The table at the right summarizes the symptoms of ethanol consumption. Small doses of ethanol, in general, produce euphoria and relaxation; people experiencing these symptoms tend to become talkative and less inhibited, and may exhibit poor judgment. At higher dosages (BAC > 1 g/L), ethanol acts as a central nervous system depressant, producing at progressively higher dosages, impaired sensory and motor function, slowed cognition, stupefaction, unconsciousness, and possible death.
Ethanol acts in the central nervous system primarily by binding to the GABAA receptor, increasing the effects of the inhibitory neurotransmitter GABA (i.e., it is a positive allosteric modulator).[30]
Prolonged heavy consumption of alcohol can cause significant permanent damage to the brain and other organs. See Alcohol consumption and health.
According to the US National Highway Traffic Safety Administration, in 2002 about "41% of people fatally injured in traffic crashes were in alcohol related crashes".[31] The risk of a fatal car accident increases exponentially with the level of alcohol in the driver's blood.[32] Most drunk driving laws governing the acceptable levels in the blood while driving or operating heavy machinery set typical upper limits of blood alcohol content (BAC) between 0.02% and 0.08%.[citation needed]
Discontinuing consumption of alcohol after several years of heavy drinking can also be fatal. Alcohol withdrawal can cause anxiety, autonomic dysfunction, seizures, and hallucinations. Delirium tremens is a condition that requires people with a long history of heavy drinking to undertake an alcohol detoxification regimen.
The reinforcing effects of alcohol consumption are also mediated by acetaldehyde generated by catalase and other oxidizing enzymes such as cytochrome P-4502E1 in the brain.[33] Although acetaldehyde has been associated with some of the adverse and toxic effects of ethanol, it appears to play a central role in the activation of the mesolimbic dopamine system.[34]
Effects on metabolism
Main articles: Ethanol metabolism and Alcohol dehydrogenase
Ethanol within the human body is converted into acetaldehyde by alcohol dehydrogenase and then into the acetyl in acetyl CoA by acetaldehyde dehydrogenase. Acetyl CoA is the final product of both carbohydrate and fat metabolism, where the acetyl can be further used to produce energy or for biosynthesis. As such, ethanol can be compared to an energy-bearing macronutrient, yielding approximately 7 kcal per gram consumed.[35] However, the product of the first step of this breakdown, acetaldehyde,[36] is more toxic than ethanol. Acetaldehyde is linked to most of the clinical effects of alcohol. It has been shown to increase the risk of developing cirrhosis of the liver[37] and multiple forms of cancer.
During the metabolism of alcohol via the respective dehydrogenases, NAD (Nicotinamide adenine dinucleotide) is converted into reduced NAD. Normally, NAD is used to metabolise fats in the liver, and as such alcohol competes with these fats for the use of NAD. Prolonged exposure to alcohol means that fats accumulate in the liver, leading to the term 'fatty liver'. Continued consumption (such as in alcoholism) then leads to cell death in the hepatocytes as the fat stores reduce the function of the cell to the point of death. These cells are then replaced with scar tissue, leading to the condition called cirrhosis.
Drug interactions
Ethanol can intensify the sedation caused by other central nervous system depressant drugs such as barbiturates, benzodiazepines, opioids, non-benzodiazepines (such as Zolpidem and Zopiclone), antipsychotics, sedative antihistamines, and antidepressants.[29] It interacts with cocaine in vivo to produce cocaethylene, another psychoactive substance.[38] Ethanol enhances the bioavailability of methylphenidate (elevated plasma d-MPH).[39] In combination with cannabis, ethanol increases plasma THC levels, which suggets that ethanol may increase the absorption of THC.[40]
Alcohol and metronidazole
One of the most important drug/food interactions that should be noted is between alcohol and metronidazole.
Metronidazole is an antibacterial agent that kills bacteria by damaging cellular DNA and hence cellular function.[41] Metronidazole is usually given to people who have diarrhea caused by Clostridium difficile bacteria. C. difficile is one of the most common microorganisms that cause diarrhea and can lead to complications such as colon inflammation and even more severely, death.
Patients who are taking metronidazole are strongly advised to avoid alcohol, even after 1 hour after the last dose. The reason is that alcohol and metronidazole can lead to side effects such as flushing, headache, nausea, vomiting, abdominal cramps, and sweating.[42][43][43] These symptoms are often called the disulfiram-like reaction. The proposed mechanism of action for this interaction is that metronidazole can bind to an enzyme that normally metabolizes alcohol. Binding to this enzyme may impair the liver's ability to process alcohol for proper excretion.[44]
Alcohol and digestion
A part of ethyl alcohol is hydrophobic. This hydrophobic or lipophilic end can diffuse across cells that line the stomach wall. In fact, alcohol is one of the rare substances that can be absorbed in the stomach. Most food substances are absorbed in the small intestine. However, even though alcohol can be absorbed in the stomach, it is mostly absorbed in the small intestine because the small intestine has a large surface area that promotes absorption. Once alcohol is absorbed in the small intestine, it delays the release of stomach contents from emptying into the small intestine. Thus, alcohol can delay the rate of absorption of nutrients.[45] After absorption, alcohol reaches the liver where it is metabolized.
Breathalyzers
Alcohol that is not processed by the liver goes to the heart. The liver can process only a certain amount of alcohol per unit time. Thus, when a person drinks too much alcohol, more alcohol can reach the heart. In the heart, alcohol reduces the force of heart contractions. Consequently, the heart will pump less blood, lowering overall body blood pressure.[46] Also, blood that reaches the heart goes to the lungs to replenish blood's oxygen concentration. It is at this stage that a person can breathe out traces of alcohol.[46] This is the underlying principle of the alcohol breath testing (or breathalyzers) to determine if a driver has been drinking and driving.[47]
From the lungs, blood returns to the heart and will be distributed throughout the body. Interestingly, alcohol increases levels of high-density lipoproteins(HDLs), which carry cholesterol.[46] Alcohol is known to make blood less likely to clot, reducing risk of heart attack and stroke. This could be the reason why alcohol could produce health benefits when consumed in moderate amounts.[48] Also, alcohol dilates blood vessels. Consequently, a person will feel warmer, and their face turns flush and pink.[46]
Loss of balance
When alcohol reaches the brain, it has the ability to delay signals that are sent between nerve cells that control balance, thinking and movement.[46]
Frequent urination
Moreover, alcohol can affect the brain's ability to produce antidiuretic hormones. These hormones are responsible for controlling the amount of urine that is produced. Alcohol prevents the body from reabsorbing water, and consequently a person who recently drank alcohol will urinate frequently.[46]
Alcohol and gastrointestinal diseases
Alcohol stimulates gastric juice production, even when food is not present. In other words, when a person drinks alcohol, the alcohol will stimulate stomach's acidic secretions that are intended to digest protein molecules. Consequently, the acidity has potential to harm the inner lining of the stomach. Normally, the stomach lining is protected by a mucus layer that prevents any acids from reaching the stomach cells.
However, in patients who have a peptic ulcer disease (PUD), this mucus layer is broken down. PUD is commonly associated with a bacteria H. pylori. H. pylori secretes a toxin that weakens the mucosal wall. As a result, acid and protein enzymes penetrate the weakened barrier. Because alcohol stimulates a person's stomach to secrete acid, a person with PUD should avoid drinking alcohol on an empty stomach. Drinking alcohol would cause more acid release to damage the weakened stomach wall.[49] Complications of this disease could include a burning pain in the abdomen, bloating and in severe cases, the presence of dark black stools indicate internal bleeding.[50] A person who drinks alcohol regularly is strongly advised to reduce their intake to prevent PUD aggravation.[50]
Magnitude of effects
Some individuals have less effective forms of one or both of the metabolizing enzymes, and can experience more severe symptoms from ethanol consumption than others. However, those having acquired alcohol tolerance have a greater quantity of these enzymes, and metabolize ethanol more rapidly.[51]
Long-term
Main article: Long-term effects of alcohol
Birth defects
Ethanol is classified as a teratogen. See fetal alcohol syndrome and fetal alcohol spectrum disorder.
Cancer
IARC list ethanol in alcoholic beverages as Group 1 carcinogens and arguments "There is sufficient evidence for the carcinogenicity of acetaldehyde (the major metabolite of ethanol) in experimental animals.".[52]
Other effects
Frequent drinking of alcoholic beverages has been shown to be a major contributing factor in cases of elevated blood levels of triglycerides.[53]
Ethanol is also widely used, clinically and over the counter, as an antitussive agent.[54]
History
For more details on this topic, see Distilled beverage.
The fermentation of sugar into ethanol is one of the earliest biotechnologies employed by humans. The intoxicating effects of ethanol consumption have been known since ancient times. Ethanol has been used by humans since prehistory as the intoxicating ingredient of alcoholic beverages. Dried residue on 9,000-year-old pottery found in China suggests that Neolithic people consumed alcoholic beverages.[55]
Although distillation was well known by the early Greeks and Arabs, the first recorded production of alcohol from distilled wine was by the School of Salerno alchemists in the 12th century.[56] The first to mention absolute alcohol, in contrast with alcohol-water mixtures, was Raymond Lull.[56]
In 1796, German-Russian chemist Johann Tobias Lowitz obtained pure ethanol by mixing partially purified ethanol (the alcohol-water azeotrope) with an excess of anhydrous alkali and then distilling the mixture over low heat.[57] French chemist Antoine Lavoisier described ethanol as a compound of carbon, hydrogen, and oxygen, and in 1807 Nicolas-Théodore de Saussure determined ethanol's chemical formula.[58][59] Fifty years later, Archibald Scott Couper published the structural formula of ethanol. It was one of the first structural formulas determined.[60]
Ethanol was first prepared synthetically in 1825 by Michael Faraday. He found that sulfuric acid could absorb large volumes of coal gas.[61] He gave the resulting solution to Henry Hennell, a British chemist, who found in 1826 that it contained "sulphovinic acid" (ethyl hydrogen sulfate).[62] In 1828, Hennell and the French chemist Georges-Simon Sérullas independently discovered that sulphovinic acid could be decomposed into ethanol.[63][64] Thus, in 1825 Faraday had unwittingly discovered that ethanol could be produced from ethylene (a component of coal gas) by acid-catalyzed hydration, a process similar to current industrial ethanol synthesis.[65]
Ethanol was used as lamp fuel in the United States as early as 1840, but a tax levied on industrial alcohol during the Civil War made this use uneconomical. The tax was repealed in 1906.[66] Use as an automotive fuel dates back to 1908, with the Ford Model T able to run on petrol(gasoline) or ethanol.[67] It remains a common fuel for spirit lamps.
Ethanol intended for industrial use is often produced from ethylene.[68] Ethanol has widespread use as a solvent of substances intended for human contact or consumption, including scents, flavorings, colorings, and medicines. In chemistry, it is both a solvent and a feedstock for the synthesis of other products. It has a long history as a fuel for heat and light, and more recently as a fuel for internal combustion engines.
Properties
Physical properties
Ethanol burning with its spectrum depicted
Ethanol is a volatile, colorless liquid that has a slight odor. It burns with a smokeless blue flame that is not always visible in normal light.
The physical properties of ethanol stem primarily from the presence of its hydroxyl group and the shortness of its carbon chain. Ethanol's hydroxyl group is able to participate in hydrogen bonding, rendering it more viscous and less volatile than less polar organic compounds of similar molecular weight, such as propane.
Ethanol is slightly more refractive than water, having a refractive index of 1.36242 (at λ=589.3 nm and 18.35 °C or 65.03 °F).[69]
The triple point for ethanol is 150 K at a pressure of 4.3 × 10−4 Pa.[70]
Solvent properties
Ethanol is a versatile solvent, miscible with water and with many organic solvents, including acetic acid, acetone, benzene, carbon tetrachloride, chloroform, diethyl ether, ethylene glycol, glycerol, nitromethane, pyridine, and toluene.[69][71] It is also miscible with light aliphatic hydrocarbons, such as pentane and hexane, and with aliphatic chlorides such as trichloroethane and tetrachloroethylene.[71]
Ethanol's miscibility with water contrasts with the immiscibility of longer-chain alcohols (five or more carbon atoms), whose water miscibility decreases sharply as the number of carbons increases.[72] The miscibility of ethanol with alkanes is limited to alkanes up to undecane: mixtures with dodecane and higher alkanes show a miscibility gap below a certain temperature (about 13 °C for dodecane[73]). The miscibility gap tends to get wider with higher alkanes and the temperature for complete miscibility increases.
Ethanol-water mixtures have less volume than the sum of their individual components at the given fractions. Mixing equal volumes of ethanol and water results in only 1.92 volumes of mixture.[69][74] Mixing ethanol and water is exothermic, with up to 777 J/mol[75] being released at 298 K.
Mixtures of ethanol and water form an azeotrope at about 89 mole-% ethanol and 11 mole-% water[76] or a mixture of 95.6 percent ethanol by mass (or about 97% alcohol by volume) at normal pressure, which boils at 351K (78 °C). This azeotropic composition is strongly temperature- and pressure-dependent and vanishes at temperatures below 303 K.[77]
Hydrogen bonding in solid ethanol at −186 °C
Hydrogen bonding causes pure ethanol to be hygroscopic to the extent that it readily absorbs water from the air. The polar nature of the hydroxyl group causes ethanol to dissolve many ionic compounds, notably sodium and potassium hydroxides, magnesium chloride, calcium chloride, ammonium chloride, ammonium bromide, and sodium bromide.[71] Sodium and potassium chlorides are slightly soluble in ethanol.[71] Because the ethanol molecule also has a nonpolar end, it will also dissolve nonpolar substances, including most essential oils[78] and numerous flavoring, coloring, and medicinal agents.
The addition of even a few percent of ethanol to water sharply reduces the surface tension of water. This property partially explains the "tears of wine" phenomenon. When wine is swirled in a glass, ethanol evaporates quickly from the thin film of wine on the wall of the glass. As the wine's ethanol content decreases, its surface tension increases and the thin film "beads up" and runs down the glass in channels rather than as a smooth sheet.
Flammability
An ethanol-water solution that contains 40% ABV (alcohol by volume) will catch fire if heated to about 26 °C (79 °F) and if an ignition source is applied to it. This is called its flash point.[79] The flash point of pure ethanol is 16.60 °C (61.88 °F), less than average room temperature.
The flash points of ethanol concentrations from 10% ABV to 96% ABV are shown below:[80]
- 10% — 49 °C (120 °F)
- 20% — 36 °C (97 °F)
- 30% — 29 °C (84 °F)
- 40% — 26 °C (79 °F)
- 50% — 24 °C (75 °F)
- 60% — 22 °C (72 °F)
- 70% — 21 °C (70 °F)
- 80% — 20 °C (68 °F)
- 90% — 17 °C (63 °F)
- 96% — 17 °C (63 °F)
Alcoholic beverages that have a low concentration of ethanol will burn if sufficiently heated and an ignition source (such as an electric spark or a match) is applied to them. For example, the flash point of ordinary wine containing 12.5% ethanol is about 52 °C (126 °F).[81]
Dishes using burning alcohol for culinary effects are called Flambé.
Production
94% denatured ethanol sold in a bottle for household use
Ethanol is produced both as a petrochemical, through the hydration of ethylene and, via biological processes, by fermenting sugars with yeast.[82] Which process is more economical depends on prevailing prices of petroleum and grain feed stocks.
Ethylene hydration
Ethanol for use as an industrial feedstock or solvent (sometimes referred to as synthetic ethanol) is made from petrochemical feed stocks, primarily by the acid-catalyzed hydration of ethylene:
- C
2H
4 + H
2O → CH
3CH
2OH
The catalyst is most commonly phosphoric acid,[83][84] adsorbed onto a porous support such as silica gel or diatomaceous earth. This catalyst was first used for large-scale ethanol production by the Shell Oil Company in 1947.[85] The reaction is carried out in the presence of high pressure steam at 300 °C (572 °F) where a 1.0:0.6 ethylene to steam ratio is maintained [86] [87]. Although it would seem like an excess of steam would generate greater yields and reaction rates, in reality the extra steam can act to dissolve the catalyst and render it useless. In the U.S., this process was used on an industrial scale by Union Carbide Corporation and others, but now only LyondellBasell uses it commercially.
In an older process, first practiced on the industrial scale in 1930 by Union Carbide,[88] but now almost entirely obsolete, ethylene was hydrated indirectly by reacting it with concentrated sulfuric acid to produce ethyl sulfate, which was hydrolyzed to yield ethanol and regenerate the sulfuric acid:[89]
- C
2H
4 + H
2SO
4 → CH
3CH
2SO
4H
- CH
3CH
2SO
4H + H
2O → CH
3CH
2OH + H
2SO
4
Fermentation
Main article: Ethanol fermentation
See also: Yeast in winemaking
Ethanol for use in alcoholic beverages, and the vast majority of ethanol for use as fuel,[90] is produced by fermentation. When certain species of yeast (e.g., Saccharomyces cerevisiae) metabolize sugar in reduced-oxygen conditions they produce ethanol and carbon dioxide. The chemical equations below summarize the conversion:
- C
6H
12O
6 → 2 CH
3CH
2OH + 2 CO2
- C
12H
22O
11 + H
2O → 4 CH
3CH
2OH + 4 CO2
Fermentation is the process of culturing yeast under favorable thermal conditions to produce alcohol. This process is carried out at around 35–40 °C (95–104 °F). Toxicity of ethanol to yeast limits the ethanol concentration obtainable by brewing; higher concentrations, therefore, are usually obtained by fortification or distillation. The most ethanol-tolerant strains of yeast can survive up to approximately 18% ethanol by volume (Red Star Pasteur Champagne wine yeast, Lalvin EC-1118 wine yeast) and 20% or greater using "Turbo Yeast" as sold for spirit and fuel distillation.
To produce ethanol from starchy materials such as cereal grains, the starch must first be converted into sugars. In brewing beer, this has traditionally been accomplished by allowing the grain to germinate, or malt, which produces the enzyme amylase. When the malted grain is mashed, the amylase converts the remaining starches into sugars. For fuel ethanol, the hydrolysis of starch into glucose can be accomplished more rapidly by treatment with dilute sulfuric acid, fungally produced amylase, or some combination of the two.[91]
Cellulose
Main article: Cellulosic ethanol
Sugars for ethanol fermentation can be obtained from cellulose.[92][93] Until recently, however, the cost of the cellulase enzymes capable of hydrolyzing cellulose has been prohibitive. The Canadian firm Iogen brought the first cellulose-based ethanol plant on-stream in 2004.[94] Its primary consumer so far has been the Canadian government, which, along with the United States Department of Energy, has invested heavily in the commercialization of cellulosic ethanol. Deployment of this technology could turn a number of cellulose-containing agricultural by-products, such as corncobs, straw, and sawdust, into renewable energy resources. Other enzyme companies are developing genetically engineered fungi that produce large volumes of cellulase, xylanase, and hemicellulase enzymes. These would convert agricultural residues such as corn stover, wheat straw, and sugar cane bagasse and energy crops such as switchgrass into fermentable sugars.[95]
Cellulose-bearing materials typically contain other polysaccharides, including hemicellulose. Hydrolysis of hemicellulose gives mostly five-carbon sugars such as xylose. S. cerevisiae, the yeast most commonly used for ethanol production, cannot metabolize xylose. Other yeasts and bacteria are under investigation to ferment xylose and other pentoses into ethanol.
Hydrocarbon
A process developed and marketed by Celanese Corporation under the name TCX Technology uses hydrocarbons such as natural gas or coal for ethanol production rather than using fermented crops such as corn or sugarcane.[96]
Testing
Infrared reflection spectra of liquid ethanol, showing the -OH band centered at ~3300 cm
−1 and C-H bands at ~2950 cm
−1.
Near infrared spectrum of liquid ethanol.
Breweries and biofuel plants employ two methods for measuring ethanol concentration. Infrared ethanol sensors measure the vibrational frequency of dissolved ethanol using the CH band at 2900 cm−1. This method uses a relatively inexpensive solid state sensor that compares the CH band with a reference band to calculate the ethanol content. The calculation makes use of the Beer-Lambert law. Alternatively, by measuring the density of the starting material and the density of the product, using a hydrometer, the change in specific gravity during fermentation indicates the alcohol content. This inexpensive and indirect method has a long history in the beer brewing industry.
Research
Further information: Ethanol research
Research on ethanol production includes working from alternative source materials, novel catalysts and new chemical processes.
Purification
Distillation
Ethylene hydration or brewing produces an ethanol–water mixture. For most industrial and fuel uses, the ethanol must be purified. Fractional distillation can concentrate ethanol to 95.6% by volume (89.5 mole%). This mixture is an azeotrope with a boiling point of 78.1 °C (172.6 °F), and cannot be further purified by distillation. Addition of an entraining agent, such as benzene, cyclohexane, or heptane, allows a new ternary azeotrope comprising the ethanol, water, and the entraining agent to be formed. This lower-boiling ternary azeotrope is removed preferentially, leading to water-free ethanol.[84]
At pressures less than atmospheric pressure, the composition of the ethanol-water azeotrope shifts to more ethanol-rich mixtures, and at pressures less than 70 torr (9.333 kPa), there is no azeotrope, and it is possible to distill absolute ethanol from an ethanol-water mixture. While vacuum distillation of ethanol is not presently economical, pressure-swing distillation is a topic of current research. In this technique, a reduced-pressure distillation first yields an ethanol-water mixture of more than 95.6% ethanol. Then, fractional distillation of this mixture at atmospheric pressure distills off the 95.6% azeotrope, leaving anhydrous ethanol at the bottom.[citation needed]
Molecular sieves and desiccants
Molecular sieves can be used to selectively absorb the water from the 95.6% ethanol solution. Synthetic zeolite in pellet form can be used, as well as a variety of plant-derived absorbents, including cornmeal, straw, and sawdust. The zeolite bed can be regenerated essentially an unlimited number of times by drying it with a blast of hot carbon dioxide. Cornmeal and other plant-derived absorbents cannot readily be regenerated, but where ethanol is made from grain, they are often available at low cost. Absolute ethanol produced this way has no residual benzene, and can be used to fortify port and sherry in traditional winery operations.
Apart from distillation, ethanol may be dried by addition of a desiccant, such as molecular sieves, cellulose, and cornmeal. The desiccants can be dried and reused.[84]
Membranes and reverse osmosis
Membranes can also be used to separate ethanol and water. Membrane-based separations are not subject to the limitations water-ethanol azeotrope because separation is not based on vapor-liquid equilibria. Membranes are often used in the so-called hybrid membrane distillation process. This process uses a pre-concentration distillation column as first separating step. The further separation is then accomplished with a membrane operated either in vapor permeation or pervaporation mode. Vapor permeation uses a vapor membrane feed and pervaporation uses a liquid membrane feed.
Other techniques
A variety of other techniques have been discussed, including the following:[84]
- Liquid-liquid extraction of ethanol from an aqueous solution;
- Extraction of ethanol from grain mash by supercritical carbon dioxide;
- Pervaporation;
- Pressure swing adsorption.[97]
Grades of ethanol
Ethanol is available in a range of purities that result from its production or, in the case of denatured alcohol, are introduced intentionally.
Denatured alcohol
Main article: Denatured alcohol
Pure ethanol and alcoholic beverages are heavily taxed as psychoactive drugs, but ethanol has many uses that do not involve consumption by humans. To relieve the tax burden on these uses, most jurisdictions waive the tax when an agent has been added to the ethanol to render it unfit to drink. These include bittering agents such as denatonium benzoate and toxins such as methanol, naphtha, and pyridine. Products of this kind are called denatured alcohol.[98][99]
Absolute alcohol
Absolute or anhydrous alcohol refers to ethanol with a low water content. There are various grades with maximum water contents ranging from 1% to a few parts per million (ppm) levels. If azeotropic distillation is used to remove water, it will contain trace amounts of the material separation agent (e.g. benzene).[100] Absolute alcohol is not intended for human consumption. Absolute ethanol is used as a solvent for laboratory and industrial applications, where water will react with other chemicals, and as fuel alcohol. Spectroscopic ethanol is an absolute ethanol with a low absorbance in ultraviolet and visible light, fit for use as a solvent in ultraviolet-visible spectroscopy.[101]
Pure ethanol is classed as 200 proof in the U.S., equivalent to 175 degrees proof in the UK system.[102]
Rectified spirits
Rectified spirit, an azeotropic composition of 96% ethanol containing 4% water, is used instead of anhydrous ethanol for various purposes. Wine spirits are about 94% ethanol (188 proof). The impurities are different from those in 95% (190 proof) laboratory ethanol.[103]
Reactions
For more details on this topic, see Alcohol.
Ethanol is classified as a primary alcohol, meaning that the carbon its hydroxyl group attaches to has at least two hydrogen atoms attached to it as well. Many ethanol reactions occur at its hydroxyl group.
Ester formation
In the presence of acid catalysts, ethanol reacts with carboxylic acids to produce ethyl esters and water:
- RCOOH + HOCH2CH3 → RCOOCH2CH3 + H2O
This reaction, which is conducted on large scale industrially, requires the removal of the water from the reaction mixture as it is formed. Esters react in the presence of an acid or base to give back the alcohol and a salt. This reaction is known as saponification because it is used in the preparation of soap. Ethanol can also form esters with inorganic acids. Diethyl sulfate and triethyl phosphate are prepared by treating ethanol with sulfur trioxide and phosphorus pentoxide respectively. Diethyl sulfate is a useful ethylating agent in organic synthesis. Ethyl nitrite, prepared from the reaction of ethanol with sodium nitrite and sulfuric acid, was formerly used as a diuretic.
Dehydration
Strong acid desiccants cause the partial dehydration of ethanol to form diethyl ether and other byproducts. If the dehydration temperature exceeds around 160 °C (320 °F), full dehydration will occur and ethylene will be the main product.
- 2 CH3CH2OH → CH3CH2OCH2CH3 + H2O (ca. 120 °C)
- CH3CH2OH → H2C=CH2 + H2O (above 160 °C)
Combustion
Complete combustion of ethanol forms carbon dioxide and water:
- C2H5OH (l) + 3 O2 (g) → 2 CO2 (g) + 3 H2O (liq); −ΔHc = 1371 kJ/mol[104] = 29.8 kJ/g = 327 kcal/mol = 7.1 kcal/g
- C2H5OH (l) + 3 O2 (g) → 2 CO2 (g) + 3 H2O (g); −ΔHc = 1236 kJ/mol = 26.8 kJ/g = 295.4 kcal/mol = 6.41 kcal/g[105]
Specific heat = 2.44 kJ/(kg·K)
Acid-base chemistry
Ethanol is a neutral molecule and the pH of a solution of ethanol in water is nearly 7.00. Ethanol can be quantitatively converted to its conjugate base, the ethoxide ion (CH3CH2O−), by reaction with an alkali metal such as sodium:[72]
- 2 CH3CH2OH + 2 Na → 2 CH3CH2ONa + H2
or a very strong base such as sodium hydride:
- CH3CH2OH + NaH → CH3CH2ONa + H2
The acidity of water and ethanol are nearly the same, as indicated by their pKa of 15.7 and 16 respectively. Thus, sodium ethoxide and sodium hydroxide exist in an equilbrium that is closely balanced:
- CH3CH2OH + NaOH CH3CH2ONa + H2O
Halogenation
Ethanol is not used industrially as a precursor to ethyl halides, but the reactions are illustrative. Ethanol reacts with hydrogen halides to produce ethyl halides such as ethyl chloride and ethyl bromide via an SN2 reaction:
- CH3CH2OH + HCl → CH3CH2Cl + H2O
These reactions require a catalyst such as zinc chloride.[89] HBr requires refluxing with a sulfuric acid catalyst.[89] Ethyl halides can, in principle, also be produced by treating ethanol with more specialized halogenating agents, such as thionyl chloride or phosphorus tribromide.[72][89]
- CH3CH2OH + SOCl2 → CH3CH2Cl + SO2 + HCl
Upon treatment with halogens in the presence of base, ethanol gives the corresponding haloform (CHX3, where X = Cl, Br, I). This conversion is called the haloform reaction.[106] " An intermediate in the reaction with chlorine is the aldehyde called chloral:
- 4 Cl2 + CH3CH2OH → CCl3CHO + 5 HCl
Oxidation
Ethanol can be oxidized to acetaldehyde and further oxidized to acetic acid, depending on the reagents and conditions.[89] This oxidation is of no importance industrially, but in the human body, these oxidation reactions are catalyzed by the enzyme liver alcohol dehydrogenase. The oxidation product of ethanol, acetic acid, is a nutrient for humans, being a precursor to acetyl CoA, where the acetyl group can be spent as energy or used for biosynthesis.
Other uses
Motor fuel
Energy content of some fuels compared with ethanol:[107] |
Fuel type |
MJ/L |
MJ/kg |
Research
octane
number |
Dry wood (20% moisture) |
|
~19.5 |
|
Methanol |
17.9 |
19.9 |
108.7[108] |
Ethanol |
21.2[109] |
26.8[109] |
108.6[108] |
E85
(85% ethanol, 15% gasoline) |
25.2 |
33.2 |
105 |
Liquefied natural gas |
25.3 |
~55 |
|
Autogas (LPG)
(60% propane + 40% butane) |
26.8 |
50. |
|
Aviation gasoline
(high-octane gasoline, not jet fuel) |
33.5 |
46.8 |
100/130 (lean/rich) |
Gasohol
(90% gasoline + 10% ethanol) |
33.7 |
47.1 |
93/94 |
Regular gasoline/petrol |
34.8 |
44.4[110] |
min. 91 |
Premium gasoline/petrol |
|
|
max. 104 |
Diesel |
38.6 |
45.4 |
25 |
Charcoal, extruded |
50 |
23 |
|
Main article: Ethanol fuel
The largest single use of ethanol is as a motor fuel and fuel additive. More than any other major country, Brazil relies on ethanol as a motor fuel. Gasoline sold in Brazil contains at least 25% anhydrous ethanol. Hydrous ethanol (about 95% ethanol and 5% water) can be used as fuel in more than 90% of new cars sold in the country. Brazilian ethanol is produced from sugar cane and noted for high carbon sequestration.[111] The US uses Gasohol (max 10% ethanol) and E85 (85% ethanol) ethanol/gasoline mixtures.
USP grade ethanol for laboratory use.
Ethanol may also be utilized as a rocket fuel, and is currently in lightweight rocket-powered racing aircraft.[112]
Australian law limits the use of pure ethanol sourced from sugarcane waste to up to 10% in automobiles. It has been recommended that older cars (and vintage cars designed to use a slower burning fuel) have their valves upgraded or replaced.[113]
According to an industry advocacy group for promoting ethanol called the American Coalition for Ethanol, ethanol as a fuel reduces harmful tailpipe emissions of carbon monoxide, particulate matter, oxides of nitrogen, and other ozone-forming pollutants.[114] Argonne National Laboratory analyzed the greenhouse gas emissions of many different engine and fuel combinations. Comparing ethanol blends with gasoline alone, they showed reductions of 8% with the biodiesel/petrodiesel blend known as B20, 17% with the conventional E85 ethanol blend, and that using cellulosic ethanol lowers emissions 64%.[115]
Ethanol combustion in an internal combustion engine yields many of the products of incomplete combustion produced by gasoline and significantly larger amounts of formaldehyde and related species such as acetaldehyde.[116] This leads to a significantly larger photochemical reactivity that generates much more ground level ozone.[117] These data have been assembled into The Clean Fuels Report comparison of fuel emissions[118] and show that ethanol exhaust generates 2.14 times as much ozone as does gasoline exhaust.[citation needed] When this is added into the custom Localised Pollution Index (LPI) of The Clean Fuels Report the local pollution (pollution that contributes to smog) is 1.7 on a scale where gasoline is 1.0 and higher numbers signify greater pollution.[citation needed] The California Air Resources Board formalized this issue in 2008 by recognizing control standards for formaldehydes as an emissions control group, much like the conventional NOx and Reactive Organic Gases (ROGs).[119]
Ethanol pump station in São Paulo, Brazil where the fuel is available commercially.
World production of ethanol in 2006 was 51 gigalitres (1.3×1010 US gal), with 69% of the world supply coming from Brazil and the United States.[120] More than 20% of Brazilian cars are able to use 100% ethanol as fuel, which includes ethanol-only engines and flex-fuel engines.[121] Flex-fuel engines in Brazil are able to work with all ethanol, all gasoline or any mixture of both. In the US flex-fuel vehicles can run on 0% to 85% ethanol (15% gasoline) since higher ethanol blends are not yet allowed or efficient. Brazil supports this population of ethanol-burning automobiles with large national infrastructure that produces ethanol from domestically grown sugar cane. Sugar cane not only has a greater concentration of sucrose than corn (by about 30%), but is also much easier to extract. The bagasse generated by the process is not wasted, but is used in power plants to produce electricity.[citation needed]
A Ford Taurus "fueled by clean burning ethanol" owned by New York City.
The United States fuel ethanol industry is based largely on corn. According to the Renewable Fuels Association, as of October 30, 2007, 131 grain ethanol bio-refineries in the United States have the capacity to produce 7.0 billion US gallons (26,000,000 m3) of ethanol per year. An additional 72 construction projects underway (in the U.S.) can add 6.4 billion US gallons (24,000,000 m3) of new capacity in the next 18 months. Over time, it is believed that a material portion of the ≈150-billion-US-gallon (570,000,000 m3) per year market for gasoline will begin to be replaced with fuel ethanol.[122]
United States Postal Service vehicle running on E85, a "flex-fuel" blend in Saint Paul, Minnesota.
Sweet sorghum is a potential source of ethanol, which is suitable for growing in dryland conditions. It is being investigated by the International Crops Research Institute for the Semi-Arid Tropics (ICRISAT) for its potential to provide fuel, along with food and animal feed, in arid parts of Asia and Africa.[123] The water requirement of sweet sorghum is one-third that of sugarcane on a comparable time scale. Also, sweet sorghum requires about 22% less water than corn also known as maize. The world’s first sweet sorghum-based ethanol production distillery began commercial ethanol production in 2007 in Andhra Pradesh, India.[124]
Ethanol's high miscibility with water means that it cannot be shipped through modern pipelines like liquid hydrocarbons.[125] Mechanics have seen increased cases of damage to small engines, in particular, the carburetor, attributable to the increased water retention by ethanol in fuel.[126]
Household heating
An example of a bio-ethanol fire in the form of a traditional fireplace, using fire-proof ceramic simulated wood logs for effect.
Ethanol fuels flue-less, real flame fireplaces. Ethanol is kept in a burner containing a wick such as glass wool, a safety shield to reduce the chances of accidents and an extinguisher such as a plate or shutter to cut off oxygen.
It provides almost the same visual benefits of a real flame log or coal fire without the need to vent the fumes via a flue as ethanol produces very little hazardous carbon monoxide, and little or no noticeable scent. It does emit carbon dioxide and requires oxygen. Therefore, external ventilation of the room containing the fire is needed to ensure safe operation.
An additional benefit is that, unlike a flue based fireplace, 100% of the heat energy produced enters the room. This serves to offset some of the heat loss from an external air vent, as well as offset the relatively high cost of the fuel compared to other forms of heating.
Feedstock
Main article: § Reactions
Ethanol is an important industrial ingredient and has widespread use as a base chemical for other organic compounds. These include ethyl halides, ethyl esters, diethyl ether, acetic acid, ethyl amines, and, to a lesser extent, butadiene.
Antiseptic
Ethanol is used in medical wipes and in most common antibacterial hand sanitizer gels at a concentration of about 62% v/v as an antiseptic. Ethanol kills organisms by denaturing their proteins and dissolving their lipids and is effective against most bacteria and fungi, and many viruses, but is ineffective against bacterial spores.[127]
Solvent
Ethanol is miscible with water and is a good general purpose solvent. It is found in paints, tinctures, markers, and personal care products such as perfumes and deodorants.
Charts
Thermophysical properties of mixtures of ethanol with water and dodecane
|
|
|
Excess volume of the mixture of ethanol and water (volume contraction) |
Heat of mixing of the mixture of ethanol and water |
Vapor-liquid equilibrium of the mixture of ethanol and water (including azeotrope) |
|
|
|
Solid-liquid equilibrium of the mixture of ethanol and water (including eutecticum) |
Miscibility gap in the mixture of dodecane and ethanol |
History
Ethanol was commonly used as fuel in early bipropellant rocket (liquid propelled) vehicles, in conjunction with an oxidizer such as liquid oxygen. The German V-2 rocket of World War II, credited with beginning the space age, used ethanol, mixed with 25% of water to reduce the combustion chamber temperature.[128][129] The V-2's design team helped develop U.S. rockets following World War II, including the ethanol-fueled Redstone rocket which launched the first U.S. satellite.[130] Alcohols fell into general disuse as more efficient rocket fuels were developed.[129]
See also
|
Pharmacy and Pharmacology portal |
- 1-Propanol
- 2,2,2-Trichloroethanol
- Breathalyzer
- Butanol fuel
- Ethanol (data page)
- Cellulosic ethanol commercialization
- Ethenol
- Ethynol
- Isopropyl alcohol
- Rubbing alcohol
- Timeline of alcohol fuel
- Ethanol induced non-lamellar phases in phospholipids
References
- ^ a b "Ethanol – Compound Summary". The PubChem Project. USA: National Center for Biotechnology Information.
- ^ Ballinger, P., Long, F.A. (1960). "Acid Ionization Constants of Alcohols. II. Acidities of Some Substituted Methanols and Related Compounds1,2". Journal of the American Chemical Society 82 (4): 795. doi:10.1021/ja01489a008.
- ^ Arnett, E.M., Venkatasubramaniam, K.G. (1983). "Thermochemical acidities in three superbase systems". J. Org. Chem. 48 (10): 1569. doi:10.1021/jo00158a001.
- ^ "ChemIDplus - 64-17-5 - LFQSCWFLJHTTHZ-UHFFFAOYSA-N - Alcohol [USP] - Similar structures search, synonyms, formulas, resource links, and other chemical information.". Retrieved 13 October 2014.
- ^ "Ethanol Material Safety Data Sheet – Europe". Distill.com. Retrieved 2014-01-18.
- ^ "10th Special Report to the U.S. Congress on Alcohol and Health: Highlights from Current Research". National Institute of Health. National Institute on Alcohol Abuse and Alcoholism. June 2000. p. 134. Retrieved 21 October 2014.
The brain is a major target for the actions of alcohol, and heavy alcohol consumption has long been associated with brain damage. Studies clearly indicate that alcohol is neurotoxic, with direct effects on nerve cells. Chronic alcohol abusers are at additional risk for brain injury from related causes, such as poor nutrition, liver disease, and head trauma.
- ^ Brust, John C.M. (4 April 2010). "Ethanol and Cognition: Indirect Effects, Neurotoxicity and Neuroprotection: A Review". International Journal of Environmental Research and Public Health. Int. J. Environ. Res. Public Health. pp. 1540–1557. doi:10.3390/ijerph7041540. Retrieved 21 October 2014.
Ethanol affects cognition in a number of ways. Indirect effects include intoxication, withdrawal, brain trauma, central nervous system infection, hypoglycemia, hepatic failure, and Marchiafava-Bignami disease. Nutritional deficiency can cause pellagra and Wernicke-Korsakoff disorder. Additionally, ethanol is a direct neurotoxin and in sufficient dosage can cause lasting dementia. However, ethanol also has neuroprotectant properties and in low-to-moderate dosage reduces the risk of dementia, including Alzheimer type.
- ^ Liebig, Justus (1834) "Ueber die Constitution des Aethers und seiner Verbindungen" (On the constitution of ether and its compounds), Annalen der Pharmacie, 9 : 1–39. From page 18: "Bezeichnen wir die Kohlenwasserstoffverbindung 4C + 10H als das Radikal des Aethers mit E2 und nennen es Ethyl, …" (Let us designate the hydrocarbon compound 4C + 10H as the radical of ether with E2 and name it ethyl …).
- ^ Harper, Douglas. "ethyl". Online Etymology Dictionary.
- ^ For a report on the 1892 International Conference on Chemical Nomenclature, see:
- Armstrong, Henry (1892). "The International Conference on Chemical Nomenclature". Nature 46 (1177): 56–59. doi:10.1038/046056c0.
- Armstrong's report is reprinted with the resolutions in English in: Armstrong, Henry (1892). "The International Conference on Chemical Nomenclature". The Journal of Analytical and Applied Chemistry 6: 390–400 (398).
The alcohols and the phenols will be called after the name of the hydrocarbon from which they are derived, terminated with the suffix ol (ex. pentanol, pentenol, etc.).
- ^ OED; etymonline.com
- ^ Dudley, Robert (2004). "Ethanol, Fruit Ripening, and the Historical Origins of Human Alcoholism in Primate Frugivory". Integrative Comparative Biology 44 (4): 315–323. doi:10.1093/icb/44.4.315. PMID 21676715.
- ^ Graber, Cynthia (2008). "Fact or Fiction?: Animals Like to Get Drunk". Scientific American. Retrieved 2010-07-23.
- ^ Leblová, Sylva; Sinecká, Eva and Vaníčková, Věra (1974). "Pyruvate metabolism in germinating seeds during natural anaerobiosis". Biologia Plantarum 16 (6): 406–411. doi:10.1007/BF02922229.
- ^ Schriver, A.; Schriver-Mazzuoli, L.; Ehrenfreund, P. and d’Hendecourt, L. (2007). "One possible origin of ethanol in interstellar medium: Photochemistry of mixed CO2–C2H6 films at 11 K. A FTIR study". Chemical Physics 334 (1–3): 128–137. Bibcode:2007CP....334..128S. doi:10.1016/j.chemphys.2007.02.018.
- ^ "A longitudinal study of ethanol a... [Rapid Commun Mass Spectrom. 2006] - PubMed - NCBI". Retrieved 13 October 2014.
- ^ Michaeleen Doucleff (September 17, 2013). "Auto-Brewery Syndrome: Apparently, You Can Make Beer In Your Gut". NPR.
- ^ Cordell, Barbara; McCarthy, Justin (2013). "A Case Study of Gut Fermentation Syndrome (Auto-Brewery) with Saccharomyces cerevisiae as the Causative Organism". International Journal of Clinical Medicine. pp. 309–312. doi:10.4236/ijcm.2013.47054.
- ^ a b Spanagel R (April 2009). "Alcoholism: a systems approach from molecular physiology to addictive behavior". Physiol. Rev. 89 (2): 649–705. doi:10.1152/physrev.00013.2008. PMID 19342616.
- ^ a b c Möykkynen T, Korpi ER (July 2012). "Acute effects of ethanol on glutamate receptors". Basic & Clinical Pharmacology & Toxicology 111 (1): 4–13. doi:10.1111/j.1742-7843.2012.00879.x. PMID 22429661.
- ^ Harald Sitte; Michael Freissmuth (2 August 2006). Neurotransmitter Transporters. Springer Science & Business Media. pp. 472–. ISBN 978-3-540-29784-0.
- ^ Allen-Gipson DS, Jarrell JC, Bailey KL, Robinson JE, Kharbanda KK, Sisson JH, Wyatt TA. (2009). "Ethanol Blocks Adenosine Uptake via Inhibiting the Nucleoside Transport System in Bronchial Epithelial Cells.". Alcohol Clin Exp Res. 33 (5): 791–8. doi:10.1111/j.1530-0277.2009.00897.x. PMC 2940831. PMID 19298329.
- ^ Becker, CE (2013-08-12). "The Clinical Pharmacology of Alcohol". California Medicine (Ncbi.nlm.nih.gov) 113 (3): 37–45. PMC 1501558. PMID 5457514.
- ^ McCoy, HG; Cipolle, RJ; Ehlers, SM; Sawchuk, RJ; Zaske, DE (November 1979). "Severe methanol poisoning. Application of a pharmacokinetic model for ethanol therapy and hemodialysis.". Am J Med 67 (5): 804–807. Retrieved 7 December 2014.
- ^ Minutes of Meeting. Technical Committee on Classification and Properties of Hazardous Chemical Data (January 12–13, 2010).
- ^ a b "Safety data for ethyl alcohol". Msds.chem.ox.ac.uk. 2008-05-09. Retrieved 2011-01-03.
- ^ Pohorecky LA, Brick J (1988). "Pharmacology of ethanol". Pharmacol. Ther 36 (2–3): 335–427. doi:10.1016/0163-7258(88)90109-X. PMID 3279433.
- ^ Alcohol use and safe drinking. US National Institutes of Health .
- ^ a b Yost, David A. (2002). "Acute care for alcohol intoxication" 112 (6). Postgraduate Medicine Online. Archived from the original on 2010-12-14. Retrieved 2007-09-29.
- ^ Santhakumar V, Wallner M, Otis TS (2007). "Ethanol acts directly on extrasynaptic subtypes of GABAA receptors to increase tonic inhibition". Alcohol 41 (3): 211–21. doi:10.1016/j.alcohol.2007.04.011. PMC 2040048. PMID 17591544.
- ^ Hingson R, Winter M (2003). "Epidemiology and consequences of drinking and driving". Alcohol research & health : the journal of the National Institute on Alcohol Abuse and Alcoholism 27 (1): 63–78. PMID 15301401.
- ^ Naranjo CA, Bremner KE (1993). "Behavioural correlates of alcohol intoxication". Addiction 88 (1): 25–35. doi:10.1111/j.1360-0443.1993.tb02761.x. PMID 8448514.
- ^ Karahanian, E.; Quintanilla, M. A. E.; Tampier, L.; Rivera-Meza, M.; Bustamante, D.; Gonzalez-Lira, V. C.; Morales, P.; Herrera-Marschitz, M.; Israel, Y. (2011). "Ethanol as a Prodrug: Brain Metabolism of Ethanol Mediates its Reinforcing Effects". Alcoholism: Clinical and Experimental Research 35 (4): 606–612. doi:10.1111/j.1530-0277.2011.01439.x. PMC 3142559. PMID 21332529. edit
- ^ Melis, M.; Enrico, P.; Peana, A. T.; Diana, M. (2007). "Acetaldehyde mediates alcohol activation of the mesolimbic dopamine system". European Journal of Neuroscience 26 (10): 2824–2833. doi:10.1111/j.1460-9568.2007.05887.x. PMID 18001279. edit
- ^ Nutrition Coordinating Center, University of Minnesota. "Primary Energy Sources". Regents of the University of Minnesota. Retrieved July 15, 2014.
- ^ Boggan, Bill. "Metabolism of Ethyl Alcohol in the Body". Chemases.com. Retrieved 2007-09-29.
- ^ Boggan, Bill. "Effects of Ethyl Alcohol on Organ Function". Chemases.com. Retrieved 2007-09-29.
- ^ Laizure, S. C.; Mandrell, T.; Gades, N. M.; Parker, R. B. (2003). "Cocaethylene metabolism and interaction with cocaine and ethanol: Role of carboxylesterases". Drug metabolism and disposition: the biological fate of chemicals 31 (1): 16–20. doi:10.1124/dmd.31.1.16. PMID 12485948. edit
- ^ Sakalo, V. S.; Romanenko, A. M.; Klimenko, I. A.; Persidskiĭ, IuV (1988). "Effects of chemotherapy on regional metastases of non-seminomatous tumors of the testis". Voprosy onkologii 34 (10): 1219–24. PMID 3188424. edit
- ^ Lukas, Scott E.; Orozco, Sara (2001). "Ethanol increases plasma Δ9-tetrahydrocannabinol (THC) levels and subjective effects after marihuana smoking in human volunteers". Drug and Alcohol Dependence 64 (2): 143–9. doi:10.1016/S0376-8716(01)00118-1. PMID 11543984.
- ^ Repchinsky C (ed.) (2012). Compendium of pharmaceuticals and specialties, Ottawa: Canadian Pharmacists Association.[full citation needed]
- ^ Aronson, I. K.; Rumsfield, J. A.; West, D. P.; Alexander, J.; Fischer, J. H.; Paloucek, F. P. (1987). "Evaluation of topical metronidazole gel in acne rosacea". Drug intelligence & clinical pharmacy 21 (4): 346–351. PMID 2952478. edit
- ^ a b SCS Pharmaceuticals. Flagyl® IV and Flagyl® I.V. RTU® (metronidazole hydrochloride) prescribing information (dated April 16, 1997). In: Physicians’ desk reference. 48th ed. Montvale, NJ: Medical Economics Company Inc; 1998:2563-5.
- ^ "Ethanol/metronidazole", p. 335 in Tatro DS, Olin BR, eds. Drug interaction facts. St. Louis: JB Lippincott Co, 1988, ISBN 0932686478.
- ^ Sherwood, Lauralee; Kell, Robert and Ward, Christopher (2010). Human Physiology: From Cells to Systems. Cengage Learning. ISBN 978-0-495-39184-5. [page needed]
- ^ a b c d e f How Your Body Processes Alcohol. Dummies.com. Retrieved on 2013-04-27.[unreliable source?]
- ^ How Breathalyzers work. Electronics.howstuffworks.com
- ^ "Alcohol effects on the digestive system". Alcoholrehab.com
- ^ Overview of Peptic Ulcer Disease: Etiology and Pathophysiology. Medscape.com. Retrieved on 2013-04-27.
- ^ a b Peptic Ulcer Disease (Stomach Ulcers) Cause, Symptoms, Treatments. Webmd.com. Retrieved on 2013-04-27.
- ^ Agarwal DP, Goedde HW (1992). "Pharmacogenetics of alcohol metabolism and alcoholism". Pharmacogenetics 2 (2): 48–62. doi:10.1097/00008571-199204000-00002. PMID 1302043.
- ^ http://monographs.iarc.fr/ENG/Classification/ClassificationsGroupOrder.pdf
- ^ "Triglycerides". American Heart Association. Archived from the original on 2007-08-27. Retrieved 2007-09-04.
- ^ Calesnick, B.; Vernick, H. (1971). "Antitussive activity of ethanol". Q J Stud Alcohol 32 (2): 434–441. PMID 4932255.
- ^ Roach, J. (July 18, 2005). "9,000-Year-Old Beer Re-Created From Chinese Recipe". National Geographic News. Retrieved 2007-09-03.
- ^ a b Forbes, Robert James (1948) A short history of the art of distillation, Brill, p. 89, ISBN 9004006176.
- ^ Lowitz, T. (1796) "Anzeige eines, zur volkommen Entwasserung des Weingeistes nothwendig zu beobachtenden, Handgriffs" (Report of a task that must be done for the complete dehydration of wine spirits [i.e., alcohol-water azeotrope]), (Crell's) Chemische Annalen …, vol. 1, pp. 195–204. See pp. 197–198: Lowitz dehydrated the azeotrope by mixing it with a 2:1 excess of anhydrous alkali and then distilling the mixture over low heat.
- ^ "Alcohol". 1911 Encyclopædia Britannica. LoveToKnow. Archived from the original on 2006-08-21.
- ^ de Saussure, Théodore (1807) "Mémoire sur la composition de l'alcohol et de l'éther sulfurique," Journal de physique, de chimie, d'histoire naturelle et des arts, vol. 64, pp. 316–354. In his 1807 paper, Saussure determined ethanol's composition only roughly; a more accurate analysis of ethanol appears on page 300 of his 1814 paper: de Saussure, Théodore (1814) "Nouvelles observations sur la composition de l'alcool et de l'éther sulfurique," Annales de Chimie, 89: 273–305.
- ^ Couper AS (1858). "On a new chemical theory" (online reprint). Philosophical magazine 16 (104–16). Retrieved 2007-09-03.
- ^ Faraday, M. (1825) "On new compounds of carbon and hydrogen, and on certain other products obtained during the decomposition of oil by heat," Philosophical Transactions of the Royal Society of London 115: 440–466. In a footnote on page 448, Faraday notes the action of sulfuric acid on coal gas and coal-gas distillate; specifically, "The [sulfuric] acid combines directly with carbon and hydrogen; and I find when [the resulting compound is] united with bases [it] forms a peculiar class of salts, somewhat resembling the sulphovinates [i.e., ethyl sulfates], but still different from them."
- ^ Hennell, H. (1826) "On the mutual action of sulphuric acid and alcohol, with observations on the composition and properties of the resulting compound," Philsophical Transactions of the Royal Society, vol. 116, pages 240–249. On page 248, Hennell mentions that Faraday gave him some sulfuric acid in which coal gas had dissolved and that he (Hennell) found that it contained "sulphovinic acid" (ethyl hydrogen sulfate).
- ^ Hennell, H. (1828). "On the mutual action of sulfuric acid and alcohol, and on the nature of the process by which ether is formed". Philosophical Transactions of the Royal Society of London 118: 365–371. doi:10.1098/rstl.1828.0021. On page 368, Hennell produces ethanol from "sulfovinic acid" (ethyl hydrogen sulfate).
- ^ Sérullas, Georges-Simon (1828) "De l'action de l'acide sulfurique sur l'alcool, et des produits qui en résultent" (On the action of sulfuric acid on alcohol, and products that result from it), Annales de Chimie et de Physique, vol 39, pages 152–186. On page 158, Sérullas mentions the production of alcohol from "sulfate acid d'hydrogène carboné" (hydrocarbon acid sulfate).
- ^ In 1855, the French chemist Marcellin Berthelot confirmed Faraday's discovery by preparing ethanol from pure ethylene. Marcellin Berthelot (1855) "Sur la formation de l'alcool au moyen du bicarbure d'hydrogène" (On the formation of alcohol by means of ethylene), Annales de chimie et de physique, series 3, vol. 43, pp. 385–405. (Note: The chemical formulas in Berthelot's paper are wrong because chemists at that time used the wrong atomic masses for the elements; e.g., carbon (6 instead of 12), oxygen (8 instead of 16), etc.)
- ^ Siegel, Robert (2007-02-15). "Ethanol, Once Bypassed, Now Surging Ahead". NPR. Retrieved 2007-09-22.
- ^ DiPardo, Joseph. "Outlook for Biomass Ethanol Production and Demand" (PDF). United States Department of Energy. Retrieved 2007-09-22.
- ^ Myers, Richard L.; Myers, Rusty L. (2007). The 100 most important chemical compounds: a reference guide. Westport, Conn.: Greenwood Press. p. 122. ISBN 0-313-33758-6.
- ^ a b c Lide, D. R., ed. (2000). CRC Handbook of Chemistry and Physics 81st edition. CRC press. ISBN 0-8493-0481-4.
- ^ "What is the triple point of alcohol?". Webanswers.com. 2010-12-31. [scientific citation needed]
- ^ a b c d Windholz, Martha (1976). The Merck index: an encyclopedia of chemicals and drugs (9th ed.). Rahway, N.J., U.S.A: Merck. ISBN 0-911910-26-3. [page needed]
- ^ a b c Morrison, Robert Thornton; Boyd, Robert Neilson (1972). Organic Chemistry (2nd ed.). Allyn and Bacon, inc. ISBN 0-205-08452-4. [page needed]
- ^ Dahlmann U, Schneider GM (1989). "(Liquid + liquid) phase equilibria and critical curves of (ethanol + dodecane or tetradecane or hexadecane or 2,2,4,4,6,8,8-heptamethylnonane) from 0.1 MPa to 120.0 MPa". J Chem Thermodyn 21 (9): 997. doi:10.1016/0021-9614(89)90160-2.
- ^ "Ethanol". Encyclopedia of chemical technology 9. 1991. p. 813.
- ^ Costigan MJ, Hodges LJ, Marsh KN, Stokes RH, Tuxford CW (1980). "The Isothermal Displacement Calorimeter: Design Modifications for Measuring Exothermic Enthalpies of Mixing". Aust. J. Chem 33 (10): 2103. doi:10.1071/CH9802103.
- ^ Lei Z, Wang H, Zhou R, Duan Z (2002). "Influence of salt added to solvent on extractive distillation". Chem Eng J. 87 (2): 149. doi:10.1016/S1385-8947(01)00211-X.
- ^ Pemberton RC, Mash CJ (1978). "Thermodynamic properties of aqueous non-electrolyte mixtures II. Vapour pressures and excess Gibbs energies for water + ethanol at 303.15 to 363.15 K determined by an accurate static method". J Chem Thermodyn 10 (9): 867. doi:10.1016/0021-9614(78)90160-X.
- ^ Merck Index of Chemicals and Drugs, 9th ed.; monographs 6575 through 6669
- ^ "Flash Point and Fire Point". Nttworldwide.com.
- ^ "Flash points of ethanol-based water solutions". Engineeringtoolbox.com. Retrieved June 23, 2011.
- ^ Wolke, Robert L. (5 July 2006). "Combustible Combination". Washington Post. Retrieved 27 January 2011.
- ^ Mills GA, Ecklund EE (1987). "Alcohols as Components of Transportation Fuels". Annual Review of Energy 12: 47. doi:10.1146/annurev.eg.12.110187.000403.
- ^ Roberts, John D.; Caserio, Marjorie C. (1977). Basic Principles of Organic Chemistry. W. A. Benjamin, Inc. ISBN 0-8053-8329-8. [page needed]
- ^ a b c d Naim Kosaric, Zdravko Duvnjak, Adalbert Farkas, Hermann Sahm, Stephanie Bringer-Meyer, Otto Goebel and Dieter Mayer in "Ethanol" Ullmann's Encyclopedia of Industrial Chemistry, 2011, Wiley-VCH, Weinheim. doi:10.1002/14356007.a09_587.pub2
- ^ "Ethanol". Encyclopedia of chemical technology 9. 1991. p. 82.
- ^ http://www.essentialchemicalindustry.org/chemicals/ethanol.html
- ^ http://www.chemlabs.bris.ac.uk/outreach/resources/Catalysis%20Web%20Pages%20for%20PreUniversity%20students%20V1_0.pdf
- ^ Lodgsdon, J.E (1991). "Ethanol". In Howe-Grant, Mary; Kirk, Raymond E.; Othmer, Donald F.; Kroschwitz, Jacqueline I. Encyclopedia of chemical technology 9 (4th ed.). New York: Wiley. p. 817. ISBN 0-471-52669-X.
- ^ a b c d e Streitweiser, Andrew Jr.; Heathcock, Clayton H. (1976). Introduction to Organic Chemistry. MacMillan. ISBN 0-02-418010-6.
- ^ Medium and long-term opportunities and risks of the biotechnological production of bulk chemicals from renewable resources – the potential of white biotechnology. The BREW project final report, Utrecht, September 2006. p. 4.
- ^ Badger, P.C. "Ethanol From Cellulose: A General Review." p. 17–21. In: J. Janick and A. Whipkey (eds.), Trends in new crops and new uses. ASHS Press, 2002, Alexandria, VA. Retrieved on September 2, 2007.
- ^ Taherzadeh MJ, Karimi K (2007). "Acid-based hydrolysis processes for ethanol from lignocellulosic materials: A review". BioResources 2: 472.
- ^ Taherzadeh MJ, Karimi K (2007). "Enzymatic-based hydrolysis processes for ethanol from lignocellulosic materials: A review". BioResources 2: 707.
- ^ Ritter SK (2004). "Biomass or Bust". Chemical & Engineering News 82 (22): 31. doi:10.1021/cen-v082n048.p031.
- ^ Clines, Tom (July 2006). "Brew Better Ethanol". Popular Science Online. Archived from the original on 2007-11-03.
- ^ Market access will save US from $4 gasoline, says FuelChoiceNow BiofuelsDigest, Sep. 21, 2011. Retrieved Apr. 6, 2012.
- ^ Jeong, Jun-Seong; Jeon, Hyungjin; Ko, Kyung-mo; Chung, Bongwoo; Choi, Gi-Wook (2012). "Production of anhydrous ethanol using various PSA (Pressure Swing Adsorption) processes in pilot plant". Renewable Energy 42: 41. doi:10.1016/j.renene.2011.09.027.
- ^ "U-M Program to Reduce the Consumption of Tax-free Alcohol; Denatured Alcohol a Safer, Less Expensive Alternative" (PDF). University of Michigan. Retrieved 2007-09-29.
- ^ Great Britain (2005). The Denatured Alcohol Regulations 2005. Statutory Instrument 2005 No. 1524.
- ^ Bernthsen, August; Bansal, Raj K. (2003) A textbook of organic chemistry, p. 402, ISBN 81-224-1459-1.
- ^ Christian, Gary D. (2003) Analytical chemistry, Vol. 1, Wiley, ISBN 0-471-21472-8[page needed]
- ^ Textbook Of Food & Bevrge Mgmt, Tata McGraw-Hill, 2007 ISBN 0-07-065573-1 p. 268
- ^ Kunkee, Ralph E. and Amerine, Maynard A. (1968). "Sugar and Alcohol Stabilization of Yeast in Sweet Wine". Appl Microbiol. 16 (7): 1067–75. PMC 547590. PMID 5664123.
- ^ Rossini, Frederick D. (1937). "Heats of Formation of Simple Organic Molecules". Ind. Eng. Chem. 29 (12): 1424. doi:10.1021/ie50336a024.
- ^ Calculated from heats of formation from CRC Handbook of Chemistry and Physics, 49th Edition, 1968–1969.
- ^ Chakrabartty, in Trahanovsky, Oxidation in Organic Chemistry, pp 343–370, Academic Press, New York, 1978
- ^ Appendix B, Transportation Energy Data Book from the Center for Transportation Analysis of the Oak Ridge National Laboratory
- ^ a b Eyidogan, Muharrem; Ozsezen, Ahmet Necati; Canakci, Mustafa; Turkcan, Ali (2010). "Impact of alcohol–gasoline fuel blends on the performance and combustion characteristics of an SI engine". Fuel 89 (10): 2713–2720. doi:10.1016/j.fuel.2010.01.032.
- ^ a b Thomas, George: Overview of Storage Development DOE Hydrogen Program PDF (99.6 KB). Livermore, CA. Sandia National Laboratories. 2000.
- ^ Thomas, George (2000). "Overview of Storage Development DOE Hydrogen Program". Sandia National Laboratories. Retrieved 2009-08-01.
- ^ Reel, M. (August 19, 2006) "Brazil's Road to Energy Independence", Washington Post.
- ^ Rocket Racing League Unveils New Flying Hot Rod, by Denise Chow, Space.com, 2010-04-26. Retrieved 2010-04-27.
- ^ Green, Ray. "Model T Ford Club Australia (Inc.)". Retrieved 24 June 2011.
- ^ Ethanol 101. American Coalition for Ethanol.
- ^ The Biofuels FAQs, The Biofuels Source Book, Energy Future Coalition, United Nations Foundation.
- ^ California Air Resources Board, Definition of a Low Emission Motor Vehicle in Compliance with the Mandates of Health and Safety Code Section 39037.05, second release, October 1989
- ^ Lowi, A. and Carter, W.P.L.; A Method for Evaluating the Atmospheric Ozone Impact of Actual Vehicle emissions, S.A.E. Technical Paper, Warrendale, PA; March 1990
- ^ Jones, T.T.M. (2008) The Clean Fuels Report: A Quantitative Comparison Of Motor Fuels, Related Pollution and Technologies. researchandmarkets.com
- ^ "Adoption of the Airborne Toxic Control Measure to Reduce Formaldehyde Emissions from Composite Wood Products". USA: Window and Door Manufacturers Association. July 30, 2008. Archived from the original on 2010-03-09.
- ^ "2008 World Fuel Ethanol Production". U.S.: Renewable Fuels Association.
- ^ "Tecnologia flex atrai estrangeiros". Agência Estado.
- ^ "First Commercial U.S. Cellulosic Ethanol Biorefinery Announced". Renewable Fuels Association. 2006-11-20. Retrieved May 31, 2011.
- ^ Sweet sorghum for food, feed and fuel New Agriculturalist, January 2008.
- ^ Developing a sweet sorghum ethanol value chain ICRISAT, 2013
- ^ Horn, W. and Krupp, F. (2008) Earth: The Sequel: The Race to Reinvent Energy and Stop Global Warming, W. W. Norton, p. 85, ISBN 0393068102.
- ^ Mechanics see ethanol damaging small engines, Msnbc.com, 8 January 2008
- ^ McDonnell G, Russell AD (1999). "Antiseptics and disinfectants: activity, action, and resistance". Clin. Microbiol. Rev. 12 (1): 147–79. PMC 88911. PMID 9880479.
- ^ Darling, David. "The Internet Encyclopedia of Science: V-2".
- ^ a b Braeunig, Robert A. "Rocket Propellants." (Website). Rocket & Space Technology, 2006. Retrieved on 2007-08-23.
- ^ "A Brief History of Rocketry." NASA Historical Archive, via science.ksc.nasa.gov.
Further reading
- The National Institute on Alcohol Abuse and Alcoholism maintains a database of alcohol-related health effects. ETOH Archival Database (1972–2003) Alcohol and Alcohol Problems Science Database.
- Boyce, John M., and Pittet Didier. (2003). "Hand Hygiene in Healthcare Settings". Centers for Disease Control, Atlanta, Georgia, United States.
- Onuki, Shinnosuke; Koziel, Jacek A.; van Leeuwen, Johannes; Jenks, William S.; Grewell, David; Cai, Lingshuang (June 2008). "Ethanol production, purification, and analysis techniques: a review". 2008 ASABE Annual International Meeting. Providence, RI. Retrieved February 16, 2013.
- Sci-toys website explanation of US denatured alcohol designations
- Smith, M.G., and M. Snyder. (2005). "Ethanol-induced virulence of Acinetobacter baumannii". American Society for Microbiology meeting. Volume 1 June 5 – June 9. Atlanta.
External links
|
Look up alcohol or ethanol in Wiktionary, the free dictionary. |
|
Wikimedia Commons has media related to Ethanol. |
- Alcohol (Ethanol) at The Periodic Table of Videos (University of Nottingham)
- International Labour Organization ethanol safety information
- National Pollutant Inventory – Ethanol Fact Sheet
- CDC – NIOSH Pocket Guide to Chemical Hazards – Ethyl Alcohol
- National Institute of Standards and Technology chemical data on ethanol
- ChEBI – biology related
- Chicago Board of Trade news and market data on ethanol futures
- Calculation of vapor pressure, liquid density, dynamic liquid viscosity, surface tension of ethanol
- Ethanol History A look into the history of ethanol
- ChemSub Online: Ethyl alcohol
- Industrial ethanol production process flow diagram using ethylene and sulphuric acid
Alcohols
|
|
Straight-chain
primary
alcohols (1°) |
- Methanol (C
1)
- Ethanol (C
2)
- 1-Propanol (C
3)
- n-Butanol (C
4)
- 1-Pentanol (C
5)
- 1-Hexanol (C
6)
- 1-Heptanol (C
7)
- 1-Octanol (C
8)
- 1-Nonanol (C
9)
- 1-Decanol (C
10)
- Undecanol (C
11)
- Dodecanol (C
12)
- Tridecan-1-ol (C
13)
- 1-Tetradecanol (C
14)
- Pentadecan-1-ol (C
15)
- Cetyl alcohol (C
16)
- Heptadecan-1-ol (C
17)
- Stearyl alcohol (C
18)
- Nonadecan-1-ol (C
19)
- Arachidyl alcohol (C
20)
- Heneicosan-1-ol (C
21)
- Docosanol (C
22)
- Tricosan-1-ol (C
23)
- 1-Tetracosanol (C
24)
- Pentacosan-1-ol (C
25)
- 1-Hexacosanol (C
26)
- 1-Heptacosanol (C
27)
- 1-Octacosanol (C
28)
- 1-Nonacosanol (C
29)
- Triacontanol (C
30)
- Policosanol
|
|
Other primary
alcohols |
- Isobutanol (C
4)
- Isoamyl alcohol (C
5)
- 2-Methyl-1-butanol (C
5)
- Phenethyl alcohol (C
8)
- Tryptophol (C
10)
|
|
Secondary
alcohols (2°) |
- Isopropanol (C
3)
- 2-Butanol (C
4)
- 2-Pentanol (C
5)
- 2-Hexanol (C
6)
- 2-Heptanol (C
7)
- Cyclohexanol (C
6)
|
|
Tertiary
alcohols (3°) |
- tert-Butyl alcohol (C
4)
- tert-Amyl alcohol (C
5)
- 2-Methyl-2-pentanol (C
6)
- 2-Methylhexan-2-ol (C
7)
- 2-Methylheptan-2-ol (C
8)
- 3-Methyl-3-pentanol (C
6)
- 3-Methyloctan-3-ol (C
9)
|
|
- Biochemical families
- carbohydrates
- alcohols
- glycoproteins
- glycosides
- lipids
- eicosanoids
- fatty acids / intermediates
- glycerides
- phospholipids
- sphingolipids
- steroids
- nucleic acids
- constituents / intermediates
- proteins
- amino acids / intermediates
- tetrapyrroles / intermediates
|
|
Motor fuels
|
|
Fuel types |
- Gasoline/petrol
- Diesel
- Biodiesel
- Lead Replacement Petrol
- Kerosene
- Compressed natural gas
- Hydrogen
- Ethanol
- Butanol fuel
- Racing fuel (Tetraethyllead)
|
|
Fuel additives |
- Butyl rubber
- Butylated hydroxytoluene
- 1,2-Dibromoethane
- 1,2-Dichloroethane
- Dimethyl methylphosphonate
- 2,4-Dimethyl-6-tert-butylphenol
- Dinonylnaphthylsulfonic acid
- 2,6-Di-tert-butylphenol
- Ecalene
- Ethylenediamine
- Metal deactivator
- Methyl tert-butyl ether
- Nitromethane
- Tetraethyllead
- Tetranitromethane
|
|
Fluids |
- Motor oil
- Antifreeze
- Automatic transmission fluid
- Brake fluid
- Gear oil
- Windshield washer fluid
|
|
Retail |
- Fuel card
- Full service
- MTBE controversy
- Pay at the pump
|
|
Molecules detected in outer space
|
|
Molecules |
|
|
Deuterated
molecules |
- Ammonia
- Ammonium ion
- Formaldehyde
- Formyl radical
- Heavy water
- Hydrogen cyanide
- Hydrogen deuteride
- Hydrogen isocyanide
- Methylacetylene
- N2D+
- Trihydrogen cation
|
|
Unconfirmed |
- Anthracene
- Dihydroxyacetone
- Ethyl methyl ether
- Glycine
- Graphene
- H2NCO+
- Linear C5
- Naphthalene cation
- Phosphine
- Pyrene
- Silylidine
|
|
Related |
- Abiogenesis
- Astrobiology
- Astrochemistry
- Atomic and molecular astrophysics
- Chemical formula
- Circumstellar envelope
- Cosmic dust
- Cosmic ray
- Cosmochemistry
- Diffuse interstellar band
- Extraterrestrial life
- Extraterrestrial liquid water
- Forbidden mechanism
- Helium hydride ion
- Homochirality
- Intergalactic dust
- Interplanetary medium
- Interstellar medium
- Iron–sulfur world theory
- Kerogen
- Life
- Organic compound
- Outer space
- PAH world hypothesis
- Panspermia
- Polycyclic aromatic hydrocarbon (PAH)
- RNA world hypothesis
- Spectroscopy
- Tholin
|
|
- Book:Chemistry
- Category:Astrochemistry
- Category:Molecules
- Portal:Astrobiology
- Portal:Chemistry
|
|
Antiseptics and disinfectants (D08)
|
|
Acridine derivatives |
- Ethacridine lactate
- 9-Aminoacridine
- Euflavine
|
|
Biguanides and amidines |
- Dibrompropamidine
- Chlorhexidine#
- Propamidine
- Hexamidine
- Polihexanide
|
|
Phenol and derivatives |
- Hexachlorophene
- Policresulen
- Phenol
- Triclosan
- Chloroxylenol#
- Biphenylol
- Fenticlor
|
|
Nitrofuran derivatives |
|
|
Iodine products |
- Iodine/octylphenoxypolyglycolether
- Povidone-iodine#
- Diiodohydroxypropane
|
|
Quinoline derivatives |
- Dequalinium
- Chlorquinaldol
- Oxyquinoline
- Clioquinol
|
|
Quaternary ammonium compounds |
- Benzalkonium
- Benzethonium chloride
- Cetrimonium (bromide/chloride)
- Cetylpyridinium
- Cetrimide
- Benzoxonium chloride
- Didecyldimethylammonium chloride
|
|
Mercurial products |
- Mercuric amidochloride
- Phenylmercuric borate
- Mercuric chloride
- Merbromin
- Thiomersal
- Mercuric iodide
|
|
Silver compounds |
|
|
Alcohols |
- Propanol (propyl alcohol)
- Isopropanol (isopropyl alcohol)
- Ethanol (ethyl alcohol)#
|
|
Other |
- Potassium permanganate
- Sodium hypochlorite
- Hydrogen peroxide
- Eosin
- Tosylchloramide
- Octenidine dihydrochloride
|
|
- #WHO-EM
- ‡Withdrawn from market
- Clinical trials:
- †Phase III
- §Never to phase III
|
|
Description |
- Anatomy
- Physiology
- Development
|
|
Disease |
- Infections
- Vesiculobullous
- Dermatitis and eczema
- Papulosquamous
- Urticaria and erythema
- Radiation-related
- Pigmentation
- Mucinoses
- Keratosis, ulcer, atrophy, and necrobiosis
- Vasculitis
- Fat
- Congenital
- Tumors
- nevi and melanomas
- epidermis
- dermis
- Symptoms and signs
|
|
Treatment |
- Procedures
- Drugs
- disinfectants
- emollients and protectives
- itch
- psoriasis
- other
- Wound and ulcer
|
|
|
Psychoactive substance-related disorder (F10–F19, 291–292; 303–305)
|
|
General |
- SID
- Substance intoxication / Drug overdose
- Withdrawal
- Substance-induced psychosis
- SUD
- Substance abuse
- Physical dependence / Substance dependence
|
|
Alcohol |
SID
|
Diseases
|
Neurological
disorders
|
- Alcoholic hallucinosis
- Alcohol withdrawal
- Fetal alcohol spectrum disorder (FASD)
- Fetal alcohol syndrome (FAS)
- Korsakoff's syndrome
- Wernicke–Korsakoff syndrome
- Wernicke's encephalopathy
|
|
Digestive
system
|
- Alcohol flush reaction
- Alcoholic hepatitis
- Alcoholic liver disease
|
|
Nervous
system
|
- Alcohol dementia
- Alcoholic hallucinosis
- Hangover
|
|
Cardiovascular
system
|
|
|
|
|
SUD
|
- Alcoholism
- Alcohol dependence
- Alcohol abuse
|
|
|
Opioids |
|
|
Caffeine |
- SID
- Effect of caffeine on memory
- Caffeine-induced sleep disorder
- SUD
|
|
Cannabis |
- SID
- Effects of cannabis
- Long-term effects of cannabis
- SUD
|
|
Sedative /
hypnotic |
- benzodiazepine: SID
- Benzodiazepine overdose
- Benzodiazepine withdrawal
- SUD
- Benzodiazepine misuse
- Benzodiazepine dependence
- barbiturate: SID
- SUD
|
|
Cocaine |
|
|
Stimulants |
|
|
Hallucinogen |
- SID
- Hallucinogen persisting perception disorder
|
|
Tobacco |
- SID
- Nicotine poisoning
- Nicotine withdrawal
|
|
Volatile
solvent |
- Inhalant abuse: Toluene toxicity
|
|
Multiple |
|
|
Index of psychology and psychiatry
|
|
Description |
|
|
Disorders |
- Mental and behavioral
- Symptoms and signs
- Evaluation and testing
|
|
Treatment |
- Psychotherapy
- Drugs
- depression
- antipsychotics
- anxiety
- dementia
- hypnotics and sedatives
- psychostimulants, ADHD drugs and nootropics
|
|
|
Alcohol and health
|
|
Ethanol
classifications |
Dependency
and harm
|
- Physical dependence
- ISCD harm and damaging rating: 72/100
- IARC Group 1 carcinogen
|
|
Pathophysiology
|
- Anxiolytic
- Depressant
- Euphoriant
- Hypnotic / sedative
|
|
|
Specific
interactions |
Note: see Template:Psychoactive substance use for diagnoses
- Aging
- Alcohol-induced mood disorders
- Brain
- Cancer
- Sleep
- Tolerance
- Weight
|
|
Substance
abuse
prevention |
Sobriety
|
- Alcohol detoxification
- Alcohol rehabilitation
- Alcoholics Anonymous
- Sober companion
|
|
Alcohol
limitation
|
- 0-0-1-3
- Ban on caffeinated alcoholic beverages
- Alcohol education
- Alcohol server training
- Recommended maximum intake of alcoholic beverages
|
|
Addiction medicine
|
Anti-addictive entheogens: Ibogaine, Salvia divinorum
|
|
Religion and alcohol
|
- Christian views on alcohol
- Islam and alcohol
- Dionysian Mysteries
|
|
|
Social issues |
- Alcohol advertising
- Alcohol-free beverage definition controversy
- Alcohol self-medication
- Native Americans
- Binge drinking
- Blackout (alcohol-related amnesia)
- College student alcoholism
- Domestic violence
- Drinking games / pregaming
- Driving under the influence
- Drunkorexia
- Dry January
- Adult Children of Alcoholics
- Family systems
- French paradox
- High-functioning alcoholic (HFA)
- Impure alcohol
- methanol outbreaks
- moonshine contamination
- Rum-running
- Sex
- Sin tax / Pigovian tax
|
|
General |
- Short-term effects of alcohol
- Long-term effects of alcohol
|
|
Other therapeutic products (V03AG–V03AZ)
|
|
Treatment of hypercalcemia |
- Sodium cellulose phosphate
|
|
Treatment of hypoglycaemia |
|
|
Medical gases |
- Oxygen
- Carbon dioxide
- Helium
- Nitrogen
|
|
Nerve depressants |
|
|
Alcoholic beverages
|
|
History and production
|
|
History of alcohol |
- History of alcoholic beverages
- History of beer
- History of wine
- History of Bordeaux wine
- History of Champagne
- History of Chianti
- History of French wine
- History of Portuguese wine
- History of Rioja wine
- History of Sherry
- History of South African wine
|
|
|
Production |
- Alcohol industry
- Brewing
- Distillation
- Drinking establishments
- Fermentation
- Winemaking
|
|
|
|
Alcoholic beverages
|
|
Fermented beverage |
- Beer
- Cider
- Mead
- Rice wine
- Sake
- Wine
- Other fermented beverages
|
|
|
Distilled beverage |
- Brandy
- Gin
- Liqueur
- Rum
- Tequila
- Vodka
- Whisky
- Other distilled beverages
|
|
Fortified wine |
- Madeira wine
- Marsala wine
- Port wine
- Sherry
- Vermouth
- Other fortified wines
|
|
|
|
Distilled beverages by ingredients
|
|
Fruit |
- Apple
- Applejack
- Calvados
- Cashew apple
- Feni
- Coconut
- Arrack
- Grape
- Armagnac
- Brandy
- Cognac
- Pisco
- Plum
- Slivovitz
- Ţuică
- Pomace
- Chacha
- Grappa
- Marc
- Orujo
- Tsikoudia
- Tsipouro
- Zivania
- Various fruits
- Eau de vie
- Kirschwasser
- Nalewka
- Pálinka
- Rakia
- Schnaps
|
|
|
Grain |
- Barley
- Irish whiskey
- Japanese whisky
- Scotch whisky
- Maize
- Bourbon whiskey
- Corn whiskey
- Tennessee whiskey
- Rice
- Awamori
- Cheongju
- Rice baijiu
- Shōchū
- Soju
- Rye
- Korn
- Rye whiskey
- Starka
- Sorghum
- Baijiu (Kaoliang)
- Multiple grains
- American whiskey
- Canadian whisky
|
|
Other |
- Agave
- Mezcal
- Tequila
- Sugarcane or molasses
- Aguardiente
- Cachaça
- Clairin
- Guaro
- Rum
- Seco Herrerano
- Tharra
- Various starches
- Akvavit
- Horilka
- Poitín
- Shōchū
- Vodka
|
|
|
|
Liqueurs and infused distilled beverages by ingredients
|
|
- Almond
- Amaretto
- Crème de Noyaux
- Anise
- Absinthe
- Arak
- Hierbas
- Herbs de Majorca
- Ouzo
- Pastis
- Rakı
- Sambuca
- Chocolate
- Chocolate liqueur
- Cinnamon
- Tentura
- Cloudberry
- Lakka
- Coconut
- Malibu
- Coffee
- Kahlua
- Tia Maria
- Egg
- Advocaat
- Hazelnut
- Frangelico
- Herbs
- Aquavit
- Bénédictine
- Brennivín
- Crème de menthe
- Metaxa
- Honey
- Bärenjäger
- Drambuie
- Glayva
- Krupnik
- Juniper
- Gin
- Jenever
- Orange
- Campari
- Curaçao
- Triple sec
- Peppers
- Pertsivka
- Star anise
- Sassolino
- Sugarcane/molasses
- Charanda
- Various fruits
- Crème de banane
- Crème de cassis
- Limoncello
- Schnapps
- Sloe gin
|
|
|
- Category
- Portals
- Beer
- Drink
- Wine
- WikiProjects
- Beer
- Spirits
- Wine
|
|
Pathophysiology of ethanol
Antidotes (V03AB)
|
|
Nervous
system |
Nerve agent /
Organophosphate
poisoning
|
- Atropine#
- Biperiden
- Diazepam#
- Oximes
- see also: Cholinesterase
|
|
Barbiturate
overdose
|
|
|
Benzodiazepine
overdose
|
|
|
GHB overdose
|
|
|
Opioid overdose
|
- Diprenorphine
- Doxapram
- Nalmefene
- Nalorphine
- Naloxone#
- Naltrexone
|
|
Reversal of
neuromuscular blockade
|
|
|
|
Circulatory
system |
Beta blocker
|
|
|
Digoxin toxicity
|
|
|
Heparin
|
|
|
|
Other |
Arsenic poisoning
|
|
|
Cyanide poisoning
|
- 4-Dimethylaminophenol
- Hydroxocobalamin
- nitrite
- Amyl nitrite
- Sodium nitrite#
- Sodium thiosulfate#
|
|
Hydrofluoric acid
|
|
|
Methanol /
Ethylene glycol
poisoning
|
- Primary alcohols: Ethanol
- Fomepizole
|
|
Paracetamol toxicity
(Acetaminophen)
|
- Acetylcysteine#
- Glutathione
- Methionine#
|
|
|
- Dimercaprol#
- Edetates
- Prussian blue#
|
|
Other
|
- iodine-131
- Methylthioninium chloride#
- oxidizing agent
- Prednisolone/promethazine
|
|
|
Emetic |
- Copper sulfate
- Ipecacuanha
|
|
- #WHO-EM
- ‡Withdrawn from market
- Clinical trials:
- †Phase III
- §Never to phase III
|
|
Description |
|
|
Disease |
|
|
Treatment |
|
|
|
Anxiolytics (N05B)
|
|
5-HT1A agonists |
|
|
GABAAR PAMs |
- Benzodiazepines:
- Adinazolam
- Alprazolam
- Bromazepam
- Camazepam
- Chlordiazepoxide
- Clobazam
- Clonazepam
- Clorazepate
- Clotiazepam
- Cloxazolam
- Diazepam#
- Ethyl loflazepate
- Etizolam
- Fludiazepam
- Halazepam
- Ketazolam
- Lorazepam#
- Medazepam
- Nordazepam
- Oxazepam
- Pinazepam
- Prazepam
- Others: Alpidem‡
- Barbiturates
- Carbamates
- Chlormezanone‡
- Ethanol
- Etifoxine; Herbs:
- Kava
- Skullcap
- Valerian
|
|
α2δ VDCC blockers |
- Gabapentin
- Gabapentin enacarbil
- Pregabalin
|
|
Antidepressants |
- SSRIs
- SNRIs
- SARIs
- TCAs
- TeCAs
- MAOIs; Others: Agomelatine
- Bupropion
- Ketamine
- Tianeptine
- Vilazodone
- Vortioxetine
|
|
Sympatholytics |
- Beta blockers
- Clonidine
- Guanfacine
- Prazosin
|
|
Others |
- Afobazole
- Baclofen
- Benzoctamine
- Cannabidiol
- Cycloserine
- Hydroxyzine
- Kanna
- Lavender
- Mebicarum
- Mepiprazole
- Opipramol
- Oxaflozane‡
- Phenaglycodol
- Phenibut
- Picamilon
- Selank
- Tiagabine
- Tofisopam
- Validolum
|
|
- #WHO-EM
- ‡Withdrawn from market
- Clinical trials:
- †Phase III
- §Never to phase III
Index of psychology and psychiatry
|
|
Description |
|
|
Disorders |
- Mental and behavioral
- Symptoms and signs
- Evaluation and testing
|
|
Treatment |
- Psychotherapy
- Drugs
- depression
- antipsychotics
- anxiety
- dementia
- hypnotics and sedatives
- psychostimulants, ADHD drugs and nootropics
|
|
|
Euphoriants
|
|
Cannabinoids |
- AM-2201
- JWH-018
- THC (found in Cannabis)
- UR-144
|
|
Depressants |
General
|
- Barbiturates
- Benzodiazepines
- GHB
- Methaqualone
- Pregabalin
- Z-drugs
|
|
Alcohols
|
- 2M2B
- Ethanol
- Ethchlorvynol
- Methylpentynol
- UMB68
|
|
Opioids
|
- 7-Hydroxymitragynine (Kratom)
- Buprenorphine
- Codeine
- Dipipanone
- Fentanyl
- Heroin
- Heterocodeine
- Hydromorphone
- Methadone
- Morphine
- Opium
- Oxycodone
- Oxymorphone
- Pethidine
|
|
|
Drugs with mixed mechanism of actions (MoA) |
- Cocaine
- Dimethyltryptamine (DMT)
- Ibogaine
- Methadone
- Pentazocine
- Tramadol
|
|
Stimulants |
General
|
Nicotine (found in Tobacco)
|
|
Releasing agents (RA)
|
- 4-Methylaminorex
- Amphetamine
- MDMA
- Mephedrone
- Methamphetamine
- Methylone
|
|
Reuptake inhibitors (RI)
|
- Cocaine
- Ethylphenidate
- Methylphenidate
|
|
|
Hallucinogens |
Deliriants
|
- Atropine
- Cyclizine
- Diphenhydramine
- Orphenadrine
- Scopolamine
- Trihexyphenidyl
|
|
Dissociatives
|
- Dextromethorphan (DXM)
- Ketamine (K)
- Methoxetamine (MXE)
- Nitrous oxide (N2O)
- Phencyclidine (PCP)
|
|
Psychedelics
|
- 2C-B
- 2C-I
- DMT
- LSD
- Mescaline
- Psilocybin
|
|
|
Hypnotics/sedatives (N05C)
|
|
GABAA |
|
|
GABAB
|
- 1,4-Butanediol
- Aceburic acid
- GABOB
- GHB (sodium oxybate)
- GBL
- GVL
|
|
H1 |
Antihistamines |
- Captodiame
- Cyproheptadine
- Diphenhydramine
- Doxylamine
- Hydroxyzine
- Methapyrilene
- Pheniramine
- Promethazine
- Propiomazine
|
|
Antidepressants |
- Tricyclic antidepressants
- Amitriptyline
- Doxepin
- Trimipramine, etc.
- Tetracyclic antidepressants
- Mianserin
- Mirtazapine, etc.
|
|
Antipsychotics |
- Typical antipsychotics
- Chlorpromazine
- Thioridazine, etc.
- Atypical antipsychotics
- Olanzapine
- Quetiapine
- Risperidone, etc.
|
|
|
α2-Adrenergic |
- Clonidine
- Detomidine
- Dexmedetomidine
- Lofexidine
- Medetomidine
- Romifidine
- Tizanidine
- Xylazine
|
|
5-HT2A |
Antidepressants |
- Trazodone
- Tricyclic antidepressants
- Amitriptyline
- Doxepin
- Trimipramine, etc.
- Tetracyclic antidepressants
- Mianserin
- Mirtazapine, etc.
|
|
Antipsychotics |
- Typical antipsychotics
- Chlorpromazine
- Thioridazine, etc.
- Atypical antipsychotics
- Olanzapine
- Quetiapine
- Risperidone, etc.
|
|
Others |
|
|
|
Melatonin |
- Agomelatine
- Melatonin
- Ramelteon
- Tasimelteon
|
|
Orexin |
- Almorexant
- Filorexant
- Suvorexant
|
|
Others |
- Acecarbromal
- Apronal
- Bromisoval
- Cannabidiol
- Carbromal
- Diethylpropanediol
- Embutramide
- Evoxine
- Fenadiazole
- Gabapentin
- Kavalactones
- Mephenoxalone
- Metaglycodol
- Niaprazine
- Opioids
- Passion flower
- Phenaglycodol
- Scopolamine
- UMB68
- Valnoctamide
|
|
Neurotoxins
|
|
Animal |
- Batrachotoxin
- Bestoxin
- Birtoxin
- Bungarotoxin
- Charybdotoxin
- Conotoxin
- Saxitoxin
- Tetrodotoxin
- Vanillotoxin
- Huwentoxin
|
|
Bacterial |
- Botulinum toxin
- Tetanospasmin
|
|
Plant |
- Penitrem A
- Picrotoxin
- Bicuculline
|
|
Pesticides |
|
|
Nerve agents |
- Cyclosarin
- EA-3148
- Novichok agent
- Sarin
- Soman
- Tabun
- VE
- VG
- VM
- VR
- VX
|
|
Physical dependants
|
|
µ-opioids |
All µ-opioids with any (even slight) agonist effect, such as (partial list) morphine, heroin, codeine, oxycodone, buprenorphine, nalbuphine, methadone, and fentanil, but not agonists specific to non-µ opioid receptors, such as salvinorin A (a k-opioid agonist), nor opioid antagonists or inverse agonists, such as naltrexone (a universal opioid inverse agonist)
|
|
GABAergics |
All GABA agonists and positive allosteric modulators of both the GABA-A ionotropic receptor and GABA-B metabotropic receptor subunits, of which the following drugs are examples (partial list):
- Alcohols
- barbiturates
- benzodiazepines
- nonbenzodiazepines (z-drugs)
- GHB
- carbamates
- baclofen
- chloral hydrate
- glutethimide
- clomethiazole
- methaqualone
|
|
Other
drug groups |
- antiepileptic
- blood pressure medications
- androgenic-anabolic steroids
- glucocorticoids
|
|
Other drugs |
- Cocaine
- gabapentin
- Nicotine
|
|
Pharmacology of ethanol
Cholinergics
|
|
Receptor ligands
|
|
mACh
|
- Agonists: 77-LH-28-1
- AC-42
- AC-260,584
- Aceclidine
- Acetylcholine
- AF30
- AF150(S)
- AF267B
- AFDX-384
- Alvameline
- AQRA-741
- Arecoline
- Bethanechol
- Butyrylcholine
- Carbachol
- CDD-0034
- CDD-0078
- CDD-0097
- CDD-0098
- CDD-0102
- Cevimeline
- Choline
- cis-Dioxolane
- Ethoxysebacylcholine
- Itameline
- LY-593,039
- L-689,660
- LY-2,033,298
- McNA343
- Methacholine
- Milameline
- Muscarine
- NGX-267
- Ocvimeline
- Oxotremorine
- PD-151,832
- Pilocarpine
- RS86
- Sabcomeline
- SDZ 210-086
- Sebacylcholine
- Suberyldicholine
- Talsaclidine
- Tazomeline
- Thiopilocarpine
- Vedaclidine
- VU-0029767
- VU-0090157
- VU-0152099
- VU-0152100
- VU-0238429
- WAY-132,983
- Xanomeline
- YM-796
- Antagonists: 3-Quinuclidinyl benzilate
- 4-DAMP
- Aclidinium bromide
- Anisodamine
- Anisodine
- Antihistamines (first-generation) (e.g., brompheniramine, chlorphenamine, cyproheptadine, dimenhydrinate, diphenhydramine, doxylamine, mepyramine (pyrilamine), phenindamine, pheniramine, promethazine, tripelennamine, triprolidine)
- Atropine
- Atropine methonitrate
- Atypical antipsychotics (e.g., clozapine, olanzapine, quetiapine, zotepine)
- Benactyzine
- Benzatropine (benztropine)
- Benzydamine
- BIBN 99
- Biperiden
- Bornaprine
- CAR-226,086
- CAR-301,060
- CAR-302,196
- CAR-302,282
- CAR-302,368
- CAR-302,537
- CAR-302,668
- CS-27349
- Cyclobenzaprine
- Cyclopentolate
- Darifenacin
- DAU-5884
- Dimethindene
- Dexetimide
- DIBD
- Dicyclomine (dicycloverine)
- Ditran
- EA-3167
- EA-3443
- EA-3580
- EA-3834
- Etanautine
- Etybenzatropine (ethybenztropine)
- Flavoxate
- Himbacine
- HL-031,120
- Ipratropium bromide
- J-104,129
- Hyoscyamine
- Mamba toxin 3
- Mamba toxin 7
- Mazaticol
- Mebeverine
- Methoctramine
- Metixene
- N-Ethyl-3-piperidyl benzilate
- N-Methyl-3-piperidyl benzilate
- Orphenadrine
- Otenzepad
- Oxybutynin
- PBID
- PD-102,807
- PD-0298029
- Phenglutarimide
- Phenyltoloxamine
- Pirenzepine
- Piroheptine
- Procyclidine
- Profenamine
- RU-47,213
- SCH-57,790
- SCH-72,788
- SCH-217,443
- Scopolamine (hyoscine)
- Solifenacin
- Telenzepine
- Tetracyclic antidepressants (e.g., amoxapine, maprotiline, mianserin, mirtazapine)
- Tiotropium bromide
- Tolterodine
- Tricyclic antidepressants (e.g., amitriptyline, butriptyline, clomipramine, desipramine, dosulepin (dothiepin), doxepin, imipramine, lofepramine, nortriptyline, protriptyline, trimipramine)
- Trihexyphenidyl
- Tripitamine
- Tropatepine
- Tropicamide
- Typical antipsychotics (e.g., chlorpromazine, loxapine, thioridazine)
- WIN-2299
- Xanomeline
- Zamifenacin
|
|
nACh
|
- Agonists: 5-HIAA
- A-84,543
- A-366,833
- A-582,941
- A-867,744
- ABT-202
- ABT-418
- ABT-560
- ABT-894
- Acetylcholine
- Altinicline
- Anabasine
- Anatoxin-a
- AR-R17779
- Butinoline
- Butyrylcholine
- Carbachol
- Choline
- Cotinine
- Cytisine
- Decamethonium
- Desformylflustrabromine
- Dianicline
- Dimethylphenylpiperazinium
- Epibatidine
- Epiboxidine
- Ethanol
- Ethoxysebacylcholine
- EVP-4473
- EVP-6124
- Galantamine
- GTS-21
- Ispronicline
- Levamisole
- Lobeline
- MEM-63,908 (RG-3487)
- Morantel
- Nicotine (tobacco)
- NS-1738
- PHA-543,613
- PHA-709,829
- PNU-120,596
- PNU-282,987
- Pozanicline
- Rivanicline
- RJR-2429
- Sazetidine A
- Sebacylcholine
- SIB-1508Y
- SIB-1553A
- SSR-180,711
- Suberyldicholine
- Suxamethonium (succinylcholine)
- TC-1698
- TC-1734
- TC-1827
- TC-2216
- TC-5214
- TC-5619
- TC-6683
- Tebanicline
- Tropisetron
- UB-165
- Varenicline
- WAY-317,538
- XY-4083
- Antagonists: 18-MAC
- 18-MC
- α-Bungarotoxin
- α-Conotoxin
- ABT-126
- Alcuronium
- Allopregnanolone
- Amantadine
- Anatruxonium
- AQW051
- Atracurium
- Bupropion
- Chandonium
- Chlorisondamine
- Cisatracurium
- Coclaurine
- Coronaridine
- Cyclopropane
- Dacuronium
- Decamethonium
- Desflurane
- Dextromethorphan
- Dextropropoxyphene
- Dextrorphan
- Diadonium
- DHβE
- Dihydrochandonium
- Dimethyltubocurarine (metocurine)
- Dipyrandium
- Dizocilpine (MK-801)
- Doxacurium
- Encenicline
- Enflurane
- Esketamine
- Fazadinium
- Gallamine
- Halothane
- Hexafluronium
- Hexamethonium (benzohexonium)
- Hydroxybupropion
- Ibogaine
- Isoflurane
- Ketamine
- Kynurenic acid
- Laudexium (laudolissin)
- Levacetylmethadol
- Levomethadone
- Malouetine
- ME-18-MC
- Mecamylamine
- Memantine
- Methadone
- Methorphan (racemethorphan)
- Methyllycaconitine
- Metocurine
- Mivacurium
- Morphanol (racemorphan)
- Neramexane
- Nitrous oxide
- Pancuronium bromide
- Pempidine
- Pentamine
- Pentolinium
- Phencyclidine
- Pipecuronium
- Progesterone
- Promegestone
- Radafaxine
- Rapacuronium
- Rocuronium
- Sevoflurane
- Surugatoxin
- Thiocolchicoside
- Toxiferine
- Tramadol
- Trimetaphan camsilate (trimethaphan camsylate)
- Tropeinium
- Tubocurarine
- Vanoxerine
- Vecuronium
- Xenon
|
|
|
|
Transporter ligands
|
|
CHT
|
- Inhibitors: Hemicholinium-3 (hemicholine)
- Triethylcholine
|
|
VAChT
|
|
|
|
|
Enzyme inhibitors
|
|
ChAT
|
- 1-(-Benzoylethyl)pyridinium
- 2-(α-Naphthoyl)ethyltrimethylammonium
- 3-Chloro-4-stillbazole
- 4-(1-Naphthylvinyl)pyridine
- Acetylseco hemicholinium-3
- Acryloylcholine
- AF64A
- B115
- BETA
- CM-54,903
- N,N-Dimethylaminoethylacrylate
- N,N-Dimethylaminoethylchloroacetate
|
|
AChE
|
|
|
BChE
|
Note: Many of the AChE inhibitors listed above also act as BChE inhibitors.
|
|
|
|
Others
|
|
Precursors
|
- Choline (lecithin)
- Citicoline
- Cyprodenate
- Dimethylethanolamine
- Glycerophosphocholine
- Meclofenoxate (centrophenoxine)
- Phosphatidylcholine
- Phosphatidylethanolamine
- Phosphorylcholine
- Pirisudanol
|
|
Cofactors
|
- Acetic acid
- Acetylcarnitine
- Acetyl-coA
- Vitamin B5
|
|
Others
|
- Acetylcholine releasing agents: α-Latrotoxin
- β-Bungarotoxin; Acetylcholine release inhibitors: Botulinum toxin (Botox); Acetylcholinesterase reactivators: Asoxime
- Obidoxime
- Pralidoxime
|
|
|
|
Glutamatergics
|
|
Receptor
(ligands) |
AMPA |
- Agonists: Glutamate/active site agonists: 5-Fluorowillardiine
- AMPA
- Domoic acid
- Glutamate
- Ibotenic acid
- Proline
- Quisqualic acid
- Willardiine; Positive allosteric modulators: Aniracetam
- Cyclothiazide
- CX-516
- CX-546
- CX-614
- Farampator (CX-691, Org 24448)
- CX-717
- CX-1739
- CX-1942
- Diazoxide
- Hydrochlorothiazide (HCTZ)
- IDRA-21
- LY-392,098
- LY-404,187
- LY-451,646
- LY-503,430
- Mibampator (LY-451,395)
- Org 26576
- Oxiracetam
- PEPA
- Piracetam
- Pramiracetam
- S-18986
- Sunifiram
- Unifiram
- Antagonists: ACEA-1011
- ATPO
- Barbiturates
- Becampanel
- Caroverine
- CNQX
- Dasolampanel
- DNQX
- Fanapanel (MPQX)
- GYKI-52466
- Licostinel (ACEA-1021)
- NBQX
- PNQX
- Selurampanel
- Tezampanel
- Topiramate
- YM90K
- Zonampanel; Negative allosteric modulators: Cyclopropane
- Enflurane
- Ethanol
- Evans blue
- GYKI-53,655
- Irampanel
- Perampanel
- Pregnenolone sulfate
- Talampanel
|
|
NMDA |
- Agonists: Glutamate/active site agonists: Aspartate
- Glutamate
- Homoquinolinic acid
- Ibotenic acid
- NMDA
- Proline
- Quinolinic acid
- Tetrazolylglycine; Glycine site agonists: ACBD
- ACPC
- ACPD
- Alanine
- CCG
- Cycloserine
- DHPG
- Fluoroalanine
- Glycine
- GLYX-13
- HA-966
- L-687,414
- Milacemide
- NRX-1074
- Sarcosine
- Serine
- Tetrazolylglycine; Polyamine site agonists: Spermidine
- Spermine
- Antagonists: Competitive antagonists: AP5 (APV)
- AP7
- CGP-37849
- CGP-39551
- CGP-39653
- CGP-40116
- CGS-19755
- CPP
- LY-233,053
- LY-235,959
- LY-274,614
- MDL-100,453
- Midafotel (d-CPPene)
- NPC-12,626
- NPC-17,742
- PBPD
- PEAQX
- Perzinfotel
- PPDA
- SDZ-220581
- Selfotel; Noncompetitive antagonists: ARR-15,896
- Caroverine
- Dexanabinol
- FPL-12495
- FR-115,427
- Hodgkinsine
- Magnesium
- MDL-27,266
- NPS-1506
- Psychotridine
- Zinc; Uncompetitive pore blockers: 2-MDP
- 3-MeO-PCP
- 8A-PDHQ
- α-Endopsychosin
- Alaproclate
- Amantadine
- Aptiganel
- ARL-12,495
- ARL-15,896-AR
- ARL-16,247
- Budipine
- Delucemine
- Dexoxadrol
- Dextrallorphan
- Dieticyclidine
- Dizocilpine
- Esketamine
- Etoxadrol
- Eticyclidine
- Gacyclidine
- Ibogaine
- Indantadol
- Ketamine
- Ketobemidone
- Lanicemine
- Loperamide
- Memantine
- Methadone (Levomethadone)
- Methorphan (Dextromethorphan
- Levomethorphan)
- Methoxetamine
- Methoxphenidine
- Milnacipran
- Morphanol (Dextrorphan
- Levorphanol)
- NEFA
- Neramexane
- Nitromemantine
- Nitrous oxide
- Noribogaine
- Orphenadrine
- PCPr
- Pethidine (meperidine)
- Phencyclamine
- Phencyclidine
- Propoxyphene
- Remacemide
- Rhynchophylline
- Rimantadine
- Rolicyclidine
- Sabeluzole
- Tenocyclidine
- Tiletamine
- Tramadol
- Xenon; Glycine site antagonists: 7-CKA
- ACC
- ACEA-1011
- ACEA-1328
- AV-101
- Carisoprodol
- CGP-39653
- DCKA
- Felbamate
- Gavestinel
- GV-196,771
- Kynurenic acid
- L-689,560
- L-701,324
- Licostinel (ACEA-1021)
- LU-73,068
- MDL-105,519
- Meprobamate
- MRZ 2/576
- PNQX
- ZD-9379; NR2B subunit antagonists: Besonprodil
- CERC-301 (MK-0657)
- CO-101,244 (PD-174,494)
- Eliprodil
- Haloperidol
- Ifenprodil
- Isoxsuprine
- Nylidrin
- Ro8-4304
- Ro25-6981
- Traxoprodil; Polyamine site antagonists: Arcaine
- Co 101676
- Diaminopropane
- Diethylenetriamine
- Huperzine A
- Putrescine
- Ro 25-6981; Unclassified/unsorted antagonists: Chloroform
- Cyclopropane
- Diethyl ether
- Diphenidine
- Enflurane
- Ethanol
- Halothane
- Isoflurane
- Methoxyflurane
- Toluene
- Trichloroethane
- Trichloroethanol
- Trichloroethylene
- Xylene
|
|
Kainate |
- Agonists: Glutamate/active site agonists: 5-Bromowillardiine
- 5-Iodowillardiine
- ATPA
- Domoic acid
- Glutamate
- Ibotenic acid
- Kainic acid
- LY-339,434
- Proline
- Quisqualic acid
- SYM-2081; Positive allosteric modulators: Cyclothiazide
- Diazoxide
- Antagonists: ACEA-1011
- CNQX
- Dasolampanel
- DNQX
- Licostinel (ACEA-1021)
- LY-382,884
- NBQX
- NS102
- Selurampanel
- Tezampanel
- Topiramate
- UBP-302; Negative allosteric modulators: Enflurane
- Ethanol
- Evans blue
- NS-3763
- Pregnenolone sulfate
|
|
mGlu1 |
- Agonists: ACPD
- DHPG
- Glutamate
- Ibotenic acid
- Quisqualic acid
- Ro01-6128
- Ro67-4853
- Ro67-7476
- VU-71
- Antagonists: BAY 36-7620
- CPCCOEt
- LY-367,385
- LY-456,236
- MCPG
- NPS-2390
|
|
mGlu2 |
- Agonists: BINA
- CBiPES
- DCG-IV
- Eglumegad
- Glutamate
- Ibotenic acid
- LY-379,268
- LY-404,039
- LY-487,379
- LY-566,332
- MGS-0028; Positive allosteric modulators: JNJ-40411813 (ADX-71149)
- Antagonists: APICA
- CECXG
- EGLU
- HYDIA
- LY-307,452
- LY-341,495
- MCPG
- MGS-0039
- PCCG-4; Negative allosteric modulators: Decoglurant
- RO4491533
|
|
mGlu3 |
- Agonists: CBiPES
- DCG-IV
- Eglumegad
- Glutamate
- Ibotenic acid
- LY-379,268
- LY-404,039
- LY-487,379
- MGS-0028
- Antagonists: APICA
- CECXG
- EGLU
- HYDIA
- LY-307,452
- LY-341,495
- MCPG
- MGS-0039; Negative allosteric modulators: Decoglurant
- RO4491533
|
|
mGlu4 |
- Agonists: Glutamate
- L-AP4
- PHCCC
- VU-001,171
- VU-0155,041; Positive allosteric modulators: MPEP
- Antagonists: CPPG
- MAP4
- MPPG
- MSOP
- MTPG
- UBP-1112
|
|
mGlu5 |
- Agonists: ACPD
- ADX-47273
- CDPPB
- CHPG
- DFB
- DHPG
- Glutamate
- Ibotenic acid
- Quisqualic acid
- VU-1545
- Antagonists: CTEP
- DMeOB
- LY-344,545
- Mavoglurant
- MCPG
- NPS-2390
- SIB-1757
- SIB-1893; Negative allosteric modulators: Basimglurant
- Dipraglurant
- Fenobam
- GRN-529
- MPEP
- MTEP
- Raseglurant
|
|
mGlu6 |
- Agonists: Glutamate
- L-AP4
- Antagonists: CPPG
- MAP4
- MPPG
- MSOP
- MTPG
- UBP-1112
|
|
mGlu7 |
- Agonists: AMN082
- Glutamate
- L-AP4
- Antagonists: CPPG
- MAP4
- MMPIP
- MPPG
- MSOP
- MTPG
- UBP-1112
|
|
mGlu8 |
- Agonists: DCPG
- Glutamate
- L-AP4
- Antagonists: CPPG
- MAP4
- MPPG
- MSOP
- MTPG
- UBP-1112
|
|
|
Transporter
(blockers) |
|
|
Enzyme
(inhibitors) |
GAH |
|
|
AST |
- 2-Amino-3-butenoic acid
- AAOA
- AMB
- β-DL-Methylene-aspartate
- Hydrazinosuccinate
|
|
ALT |
- β-Chloro-L-alanine
- L-Cycloserine
- Propargylglycine
|
|
GDH |
- AAOA
- Bithionol
- Chloroquine
- EGCG
- GTP
- GW5074
- Hexachlorophene
- Hydroxylamine
- Palmitoyl-CoA
- Pyridoxal phosphate
|
|
GS |
- 2-Aminoadipic acid
- JFD01307SC
- Methionine sulfoximine
- Phosphinothricin (glufosinate)
|
|
GAD |
- 3-Mercaptopropionic acid
- AAOA
- L-Allylglycine
- Semicarbazide
|
|
|
Others |
- Cofactors: α-Ketoglutaric acid
- Iron
- Sulfur
- Vitamin B2
- Vitamin B3
|
|
See also: GABAergics • GHBergics • Glycinergics
|
|
Serotonergics
|
|
5-HT1 receptor ligands
|
|
5-HT1A
|
- Agonists: 8-OH-DPAT
- Adatanserin
- Antidepressants (e.g., etoperidone, nefazodone, trazodone, vilazodone, vortioxetine)
- Atypical antipsychotics (e.g., aripiprazole, asenapine, clozapine, lurasidone, quetiapine, ziprasidone)
- Azapirones (e.g., buspirone, eptapirone, gepirone, perospirone, tandospirone)
- Bay R 1531
- Befiradol
- BMY-14802
- Cannabidiol
- Dimemebfe
- Ebalzotan
- Eltoprazine
- Ergolines (e.g., bromocriptine, cabergoline, dihydroergotamine, ergotamine, lisuride, LSD, methylergometrine (methylergonovine), methysergide, pergolide)
- F-11,461
- F-12,826
- F-13,714
- F-14,679
- F-15,063
- F-15,599
- Flesinoxan
- Flibanserin
- Lesopitron
- LY-293,284
- LY-301,317
- mCPP
- MKC-242
- Naluzotan
- NBUMP
- Osemozotan
- Oxaflozane
- Pardoprunox
- Piclozotan
- Rauwolscine
- Repinotan
- Roxindole
- RU-24,969
- S 14,506
- S-14,671
- S-15,535
- Sarizotan
- Serotonin (5-HT)
- SSR-181,507
- Sunepitron
- Tryptamines (e.g., 5-CT, 5-MeO-DMT, 5-MT, bufotenin, DMT, indorenate, N-Me-5-HT, psilocin, psilocybin)
- U-92,016-A
- Urapidil
- Vilazodone
- Xaliproden
- Yohimbine
- Antagonists: Atypical antipsychotics (e.g., iloperidone, risperidone, sertindole)
- AV965
- Beta blockers (e.g., alprenolol, cyanopindolol, iodocyanopindolol, oxprenolol, pindobind, pindolol, propranolol, tertatolol)
- BMY-7,378
- CSP-2503
- Dotarizine
- Ergolines (e.g., metergoline)
- Flopropione
- GR-46611
- Isamoltane
- Lecozotan
- Mefway
- Metitepine (methiothepin)
- MIN-117
- MPPF
- NAN-190
- Robalzotan
- S-15535
- SB-649,915
- SDZ 216-525
- Spiperone
- Spiramide
- Spiroxatrine
- UH-301
- WAY-100,135
- WAY-100,635
- Xylamidine
- Unknown/unsorted: Ergolines (e.g., ergometrine (ergonovine))
|
|
5-HT1B
|
- Agonists: CGS-12066A
- CP-93,129
- CP-94,253
- CP-135,807
- Eltoprazine
- Ergolines (e.g., bromocriptine, dihydroergotamine, ergotamine, methylergometrine (methylergonovine), methysergide, pergolide)
- mCPP
- RU-24,969
- Serotonin (5-HT)
- Triptans (e.g., avitriptan, donitriptan, eletriptan, sumatriptan, zolmitriptan)
- TFMPP
- Tryptamines (e.g., 5-BT, 5-CT, 5-MT, DMT)
- Vortioxetine
- Antagonists: AR-A000002
- Elzasonan
- Ergolines (e.g., metergoline)
- GR-127,935
- Isamoltane
- Metitepine (methiothepin)
- SB-216,641
- SB-224,289
- SB-236,057
- Yohimbine
- Unknown/unsorted: Ergolines (e.g., cabergoline, ergometrine (ergonovine), lisuride)
|
|
5-HT1D
|
- Agonists: CP-135,807
- CP-286,601
- Ergolines (e.g., bromocriptine, cabergoline, dihydroergotamine, ergotamine, LSD, methysergide)
- GR-46611
- L-694,247
- L-772,405
- mCPP
- PNU-109,291
- PNU-142633
- Serotonin (5-HT)
- Triptans (e.g., almotriptan, avitriptan, donitriptan, eletriptan, frovatriptan, naratriptan, rizatriptan, sumatriptan, zolmitriptan)
- Tryptamines (e.g., 5-BT, 5-CT, 5-Et-DMT, 5-MT, 5-(nonyloxy)tryptamine, DMT)
- Antagonists: Alniditan
- BRL-15,572
- Elzasonan
- Ergolines (e.g., metergoline)
- GR-127,935
- Ketanserin
- LY-310,762
- LY-367,642
- LY-456,219
- LY-456,220
- Metitepine (methiothepin)
- Mianserin
- Ritanserin
- Yohimbine
- Ziprasidone
- Unknown/unsorted: Ergolines (e.g., lisuride, lysergol, pergolide)
|
|
5-HT1E
|
- Agonists: BRL-54443
- Ergolines (e.g., methysergide)
- Serotonin (5-HT)
- Triptans (e.g., eletriptan)
- Tryptamines (e.g., tryptamine)
- Antagonists: Metitepine (methiothepin)
- Unknown/unsorted: Ergolines (e.g., ergometrine (ergonovine), lysergol, methylergometrine (methylergonovine)
|
|
5-HT1F
|
- Agonists: BRL-54443
- Ergolines (e.g., bromocriptine, lysergol, methylergometrine (methylergonovine) methysergide)
- Lasmiditan
- LY-334,370
- Serotonin (5-HT)
- Triptans (e.g., eletriptan, naratriptan, sumatriptan)
- Tryptamines (e.g., 5-MT)
- Antagonists: Mianserin
- Metitepine (methiothepin)
|
|
|
|
5-HT2 receptor ligands
|
|
5-HT2A
|
- Agonists: 25H/NB series (e.g., 25I-NBF, 25I-NBMD, 25I-NBOH, 25I-NBOMe, 25B-NBOMe, 25C-NBOMe, 25TFM-NBOMe, 2CBCB-NBOMe, 25CN-NBOH, 2CBFly-NBOMe)
- 2Cs (e.g., 2C-B, 2C-E, 2C-I, 2C-T-2, 2C-T-7, 2C-T-21)
- 2C-B-FLY
- 2CB-Ind
- 5-Methoxytryptamines (5-MeO-DET, 5-MeO-DiPT, 5-MeO-DMT, 5-MeO-DPT, 5-MT)
- α-Alkyltryptamines (e.g., 5-Cl-αMT, 5-Fl-αMT, 5-MeO-αET, 5-MeO-αMT, α-Me-5-HT, αET, αMT)
- AL-34662
- AL-37350A
- Bromo-DragonFLY
- Dimemebfe
- DOx (e.g., DOB, DOC, DOI, DOM)
- Efavirenz
- Ergolines (e.g., ALD-52, bromocriptine, cabergoline, ergine (LSA), ergotamine, lisuride, LA-SS-Az, LSB, LSD, LSD-Pip, LSH, LSP, methylergometrine (methylergonovine), pergolide)
- Jimscaline
- Juncosamine
- MDxx (e.g., MDA, MDMA, MDOH, MMDA)
- Medifoxamine
- O-4310
- Oxaflozane
- PHA-57378
- PNU-22394
- PNU-181731
- RH-34
- Phenethylamines (e.g., lophophine, mescaline)
- Piperazines (e.g., BZP, mCPP, quipazine, TFMPP)
- Serotonin (5-HT)
- TCB-2
- TFMFly
- Tryptamines (e.g., 5-BT, 5-CT, bufotenin, DET, DiPT, DMT, DPT, psilocin, psilocybin, tryptamine)
- Antagonists: 5-I-R91150
- 5-MeO-NBpBrT
- AC-90179
- Adatanserin
- Altanserin
- AMDA
- APD-215
- Atypical antipsychotics (e.g., amperozide, aripiprazole, asenapine, blonanserin, carpipramine, clocapramine, clorotepine, clozapine, fluperlapine, gevotroline, iloperidone, melperone, mosapramine, olanzapine, paliperidone, quetiapine, risperidone, sertindole, zicronapine, ziprasidone, zotepine)
- Cinanserin
- CSP-2503
- Cyproheptadine
- Deramciclane
- Dotarizine
- Eplivanserin
- Ergolines (e.g., amesergide, LY-53857, LY-215840, mesulergine, metergoline, methysergide, sergolexole)
- Etoperidone
- Fananserin
- Flibanserin
- Glemanserin
- Irindalone
- Ketanserin
- KML-010
- Lubazodone
- Mepiprazole
- Metitepine (methiothepin)
- MIN-101
- Nantenine
- Nefazodone
- Pimavanserin
- Pirenperone
- Pizotifen
- Pruvanserin
- Rauwolscine
- Ritanserin
- S-14,671
- Sarpogrelate
- Setoperone
- Spiperone
- Spiramide
- SR-46349B
- Teniloxazine
- Tetracyclic antidepressants (e.g., amoxapine, aptazapine, esmirtazapine, maprotiline, mianserin, mirtazapine)
- Trazodone
- Tricyclic antidepressants (e.g., amitriptyline)
- Typical antipsychotics (e.g., chlorpromazine, fluphenazine, haloperidol, loxapine, perphenazine, pimozide, pipamperone, prochlorperazine, thioridazine, thiothixene, trifluoperazine)
- Volinanserin
- Xylamidine
- Yohimbine
- Unknown/unsorted: Ergolines (e.g., dihydroergotamine, ergometrine (ergonovine), nicergoline)
|
|
5-HT2B
|
- Agonists: 4-Methylaminorex
- Aminorex
- Amphetamines (eg., chlorphentermine, cloforex, dexfenfluramine, fenfluramine, levofenfluramine, norfenfluramine)
- BW-723C86
- DOx (e.g., DOB, DOC, DOI, DOM)
- Ergolines (e.g., cabergoline, dihydroergocryptine, dihydroergotamine, ergotamine, methylergometrine (methylergonovine), methysergide, pergolide)
- MDxx (e.g., MDA, MDMA, MDOH, MMDA)
- Piperazines (e.g., mCPP)
- PNU-22394
- Ro60-0175
- Serotonin (5-HT)
- Tryptamines (e.g., 5-BT, 5-CT, 5-MT, α-Me-5-HT, bufotenin, DET, DiPT, DMT, DPT, psilocin, psilocybin, tryptamine)
- Antagonists: Agomelatine
- Asenapine
- Cyproheptadine
- EGIS-7625
- Ergolines (e.g., amesergide, bromocriptine, lisuride, LY-53857, LY-272015, mesulergine)
- Ketanserin
- Metadoxine
- Metitepine (methiothepin)
- Pirenperone
- Propranolol
- PRX-08066
- Rauwolscine
- Ritanserin
- RS-127,445
- Sarpogrelate
- SB-200,646
- SB-204,741
- SB-206,553
- SB-215,505
- SB-221,284
- SB-228,357
- SDZ SER-082
- Tegaserod
- Tetracyclic antidepressants (e.g., amoxapine, mianserin)
- Yohimbine
- Unknown/unsorted: Ergolines (e.g., ergometrine (ergonovine))
|
|
5-HT2C
|
- Agonists: 2Cs (e.g., 2C-B, 2C-E, 2C-I, 2C-T-2, 2C-T-7, 2C-T-21)
- 5-Methoxytryptamines (5-MeO-DET, 5-MeO-DiPT, 5-MeO-DMT, 5-MeO-DPT, 5-MT)
- α-Alkyltryptamines (e.g., 5-Cl-αMT, 5-Fl-αMT, 5-MeO-αET, 5-MeO-αMT, α-Me-5-HT, αET, αMT)
- A-372,159
- AL-38022A
- Alstonine
- CP-809,101
- Dimemebfe
- DOx (e.g., DOB, DOC, DOI, DOM)
- Ergolines (e.g., ALD-52, cabergoline, dihydroergotamine, ergine (LSA), ergotamine, lisuride, LA-SS-Az, LSB, LSD, LSD-Pip, LSH, LSP, pergolide)
- Lorcaserin
- MDxx (e.g., MDA, MDMA, MDOH, MMDA)
- Medifoxamine
- MK-212
- Org 12,962
- ORG-37,684
- Oxaflozane
- PHA-57378
- Phenethylamines (e.g., lophophine, mescaline)
- Piperazines (e.g., aripiprazole, BZP, mCPP, quipazine, TFMPP)
- PNU-22394
- PNU-181731
- Ro60-0175
- Ro60-0213
- Serotonin (5-HT)
- Tryptamines (e.g., 5-BT, 5-CT, bufotenin, DET, DiPT, DMT, DPT, psilocin, psilocybin, tryptamine)
- Vabicaserin
- WAY-629
- WAY-161,503
- YM-348
- Antagonists: Adatanserin
- Agomelatine
- Atypical antipsychotics (e.g., asenapine, clorotepine, clozapine, fluperlapine, iloperidone, melperone, olanzapine, paliperidone, quetiapine, risperidone, sertindole, ziprasidone, zotepine)
- Captodiame
- CEPC
- Cinanserin
- Cyproheptadine
- Deramciclane
- Dotarizine
- Eltoprazine
- Ergolines (e.g., amesergide, bromocriptine, LY-53857, LY-215840, mesulergine, metergoline, methysergide, sergolexole)
- Etoperidone
- Fluoxetine
- FR-260,010
- Irindalone
- Ketanserin
- Ketotifen
- Latrepirdine
- Metitepine (methiothepin)
- Nefazodone
- Pirenperone
- Pizotifen
- Propranolol
- Ritanserin
- RS-102,221
- S-14,671
- SB-200,646
- SB-206,553
- SB-221,284
- SB-228,357
- SB-242,084
- SB-243,213
- SDZ SER-082
- Tedatioxetine
- Tetracyclic antidepressants (e.g., amoxapine, aptazapine, esmirtazapine, maprotiline, mianserin, mirtazapine)
- Trazodone
- Tricyclic antidepressants (e.g., amitriptyline, nortriptyline)
- Typical antipsychotics (e.g., chlorpromazine, loxapine, pimozide, pipamperone, thioridazine)
- Xylamidine
- Unknown/unsorted: Efavirenz
- Ergolines (e.g., ergometrine (ergonovine), methylergometrine (methylergonovine))
|
|
|
|
- 5-HT3
- 5-HT4
- 5-HT5
- 5-HT6
- 5-HT7 ligands
|
|
5-HT3
|
- Agonists: Alcohols (e.g., butanol, ethanol, trichloroethanol)
- m-CPBG
- Phenylbiguanide
- Piperazines (e.g., BZP, mCPP, quipazine)
- RS-56812
- Serotonin (5-HT)
- SR-57,227
- SR-57,227-A
- Tryptamines (e.g., 2-Me-5-HT, 5-CT, bufotenidine (5-HTQ))
- Volatiles/gases (e.g., halothane, isoflurane, toluene, trichloroethane)
- YM-31636
- Antagonists: Alosetron
- AS-8112
- Atypical antipsychotics (e.g., clozapine, olanzapine, quetiapine)
- Azasetron
- Batanopride
- Bemesetron
- Cilansetron
- CSP-2503
- Dazopride
- Dolasetron
- Galanolactone
- Granisetron
- ICS-205,930
- Lerisetron
- MDL-72,222
- Memantine
- Ondansetron
- Palonosetron
- Ramosetron
- Renzapride
- Ricasetron
- Tedatioxetine
- Tetracyclic antidepressants (e.g., amoxapine, mianserin, mirtazapine)
- Thujone
- Tropanserin
- Tropisetron
- Typical antipsychotics (e.g., loxapine)
- Volatiles/gases (e.g., nitrous oxide, sevoflurane, xenon)
- Vortioxetine
- Zacopride
- Zatosetron
- Unknown/unsorted: LY-53857
- Piperazines (e.g., naphthylpiperazine)
|
|
5-HT4
|
- Agonists: 5-MT
- BIMU8
- Cinitapride
- Cisapride
- CJ-033,466
- Dazopride
- Metoclopramide
- Mosapride
- Prucalopride
- PRX-03140
- Renzapride
- RS-67333
- RS-67506
- Serotonin (5-HT)
- SL65.0155
- Tegaserod
- Velusetrag
- Zacopride
- Antagonists: GR-113,808
- GR-125,487
- L-Lysine
- Piboserod
- RS-39604
- RS-67532
- SB-203,186
- SB-204,070
|
|
5-HT5A
|
- Agonists: Ergolines (e.g., 2-Br-LSD (BOL-148), ergotamine, LSD)
- Serotonin (5-HT)
- Tryptamines (e.g., 5-CT)
- Valerenic Acid
- Antagonists: Asenapine
- Latrepirdine
- Metitepine (methiothepin)
- Ritanserin
- SB-699,551
- Unknown/unsorted: Ergolines (e.g., metergoline, methysergide)
- Piperazines (e.g., naphthylpiperazine)
|
|
5-HT6
|
- Agonists: Ergolines (e.g., dihydroergocryptine, dihydroergotamine, ergotamine, lisuride, LSD, mesulergine, metergoline, methysergide)
- Serotonin (5-HT)
- Tryptamines (e.g., 2-Me-5-HT, 5-BT, 5-CT, 5-MT, Bufotenin, E-6801, E-6837, EMD-386,088, EMDT, LY-586,713, N-Me-5-HT, tryptamine)
- WAY-181,187
- WAY-208,466
- Antagonists: ABT-354
- Atypical antipsychotics (e.g., aripiprazole, asenapine, clorotepine, clozapine, fluperlapine, iloperidone, olanzapine, tiospirone)
- AVN-101
- AVN-211
- AVN-322
- AVN-397
- BGC20-760
- BVT-5182
- BVT-74316
- Cerlapirdine
- EGIS-12,233
- GW-742,457
- Idalopirdine
- Ketanserin
- Latrepirdine
- Metitepine (methiothepin)
- MS-245
- PRX-07034
- Ritanserin
- Ro04-6790
- Ro 63-0563
- SB-258,585
- SB-271,046
- SB-357,134
- SB-399,885
- SB-742,457
- Tetracyclic antidepressants (e.g., amoxapine, mianserin)
- Tricyclic antidepressants (e.g., amitriptyline, clomipramine, doxepin, nortriptyline)
- Typical antipsychotics (e.g., chlorpromazine, loxapine)
- Unknown/unsorted: Ergolines (e.g., 2-Br-LSD (BOL-148), bromocriptine, lergotrile, pergolide)
- Piperazines (e.g., naphthylpiperazine)
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5-HT7
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- Agonists: 8-OH-DPAT
- AS-19
- Bifeprunox
- E-55888
- Ergolines (e.g., LSD)
- LP-12
- LP-44
- RU-24,969
- Sarizotan
- Serotonin (5-HT)
- Triptans (e.g., frovatriptan)
- Tryptamines (e.g., 5-CT, 5-MT, bufotenin, N-Me-5-HT)
- Antagonists: Atypical antipsychotics (e.g., amisulpride, aripiprazole, asenapine, clorotepine, clozapine, fluperlapine, olanzapine, risperidone, sertindole, tiospirone, ziprasidone, zotepine)
- Butaclamol
- DR-4485
- EGIS-12,233
- Ergolines (e.g., 2-Br-LSD (BOL-148), amesergide, bromocriptine, cabergoline, dihydroergotamine, ergotamine, LY-53857, LY-215840, mesulergine, metergoline, methysergide, sergolexole)
- Ketanserin
- LY-215,840
- Metitepine (methiothepin)
- Ritanserin
- SB-258,719
- SB-258,741
- SB-269,970
- SB-656,104
- SB-656,104-A
- SB-691,673
- SLV-313
- SLV-314
- Spiperone
- SSR-181,507
- Tetracyclic antidepressants (e.g., amoxapine, maprotiline, mianserin, mirtazapine)
- Tricyclic antidepressants (e.g., amitriptyline, clomipramine, imipramine)
- Typical antipsychotics (e.g., acetophenazine, chlorpromazine, chlorprothixene, fluphenazine, loxapine, pimozide)
- Vortioxetine
- Unknown/unsorted: Ergolines (e.g., lisuride, pergolide)
- Piperazines (e.g., naphthylpiperazine)
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Reuptake inhibitors
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SERT
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- Selective serotonin reuptake inhibitors (SSRIs): Alaproclate
- Citalopram
- Dapoxetine
- Desmethylcitalopram
- Escitalopram
- Femoxetine
- Fluoxetine
- Fluvoxamine
- Indalpine
- Ifoxetine
- Litoxetine
- Lubazodone
- Omiloxetine
- Panuramine
- Paroxetine
- Pirandamine
- RTI-353
- Seproxetine
- Sertraline
- Vilazodone
- Vortioxetine
- Zimelidine
- Serotonin-norepinephrine reuptake inhibitors (SNRIs): Bicifadine
- Desvenlafaxine
- Duloxetine
- Eclanamine
- Levomilnacipran
- Milnacipran
- N-Methyl-PPPA
- PPPA
- SEP-227162
- Sibutramine
- Venlafaxine
- Serotonin-norepinephrine-dopamine reuptake inhibitors (SNDRIs): Brasofensine
- Dasotraline
- Desmethylsertraline
- Diclofensine
- DOV-102677
- DOV-21947
- DOV-216303
- Liafensine
- NS-2359
- Perafensine
- SEP-228431
- SEP-228432
- Tedatioxetine
- Tesofensine
- Tricyclic antidepressants (TCAs): Amitriptyline
- Butriptyline
- Cianopramine
- Clomipramine
- Desipramine
- Dosulepin
- Doxepin
- Imipramine
- Lofepramine
- Nortriptyline
- Pipofezine
- Protriptyline
- Trimipramine
- Others: Amoxapine
- Antihistamines (e.g., brompheniramine, chlorphenamine, dimenhydrinate, diphenhydramine, mepyramine (pyrilamine), pheniramine, tripelennamine)
- Arylcyclohexylamines (e.g., ketamine, phencyclidine)
- CP-39,332
- Cyclobenzaprine
- Dextromethorphan
- Dextrorphan
- Efavirenz
- Etoperidone
- EXP-561
- Fezolamine
- Loxapine
- Mesembrine
- MIN-117
- N-Me-5-HT
- Nefazodone
- Nefopam
- Opioids (e.g., dextropropoxyphene, methadone, pethidine (meperidine))
- PIM-35
- Pridefine
- Roxindole
- SB-649,915
- Tofenacin
- Trazodone
- Tropanes (e.g., cocaine)
- Ziprasidone
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VMATs
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- Amiodarone
- Amphetamines (e.g., amphetamine, methamphetamine, MDMA)
- APP
- AZIK
- Bietaserpine
- Deserpidine
- Dihydrotetrabenazine
- Efavirenz
- GBR-12935
- GZ-793A
- Ibogaine
- Ketanserin
- Lobeline
- Methoxytetrabenazine
- NBI-98854
- Reserpine
- SD-809
- Tetrabenazine
- Vanoxerine (GBR-12909)
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Enzyme inhibitors
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TPH
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- AGN-2979
- Fenclonine (PCPA)
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AAAD
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- Benserazide
- Carbidopa
- Genistein
- Methyldopa
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MAO
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- Non-selective: Benmoxin
- Caroxazone
- Echinopsidine
- Furazolidone
- Hydralazine
- Indantadol
- Iproclozide
- Iproniazid
- Isocarboxazid
- Isoniazid
- Linezolid
- Mebanazine
- Metfendrazine
- Nialamide
- Octamoxin
- Paraxazone
- Phenelzine
- Pheniprazine
- Phenoxypropazine
- Pivalylbenzhydrazine
- Procarbazine
- Safrazine
- Tranylcypromine
- MAO-A-selective: Amiflamine
- Bazinaprine
- Befloxatone
- Brofaromine
- Cimoxatone
- Clorgiline
- Eprobemide
- Esuprone
- Harmala alkaloids (e.g., harmine, harmaline, harman, norharman, tetrahydroharmine)
- Methylene blue
- Metralindole
- Minaprine
- Moclobemide
- Pirlindole
- Sercloremine
- Tetrindole
- Toloxatone
- Tyrima
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Others
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Precursors
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Cofactors
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- Ferrous iron (Fe2+)
- Magnesium (Mg2+)
- Tetrahydrobiopterin
- Vitamin B3 (Niacin
- Nicotinamide → NADPH)
- Vitamin B6 (Pyridoxine
- Pyridoxamine
- Pyridoxal → Pyridoxal phosphate)
- Vitamin B9 (Folic Acid → Tetrahydrofolic acid)
- Vitamin C (Ascorbic acid)
- Zinc (Zn2+)
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Neurotoxins
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- 3-CA
- 4-CAB
- 5,7-DHT
- α-Me-DA (3,4-DHA)
- αET
- αMT
- DCA
- MDA
- MDMA
- PBA
- PCA
- PIA
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Others
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- Activity enhancers: BPAP
- PPAP
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See also
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See also: Adrenergics • Dopaminergics • Melatonergics
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