関: amphotericin B

WordNet

an antibiotic and antifungal agent
having characteristics of both an acid and a base and capable of reacting as either (同)amphiprotic

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出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2013/10/27 18:49:52」(JST)

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Amphotericin B (Fungilin, Fungizone, Abelcet, AmBisome, Fungisome, Amphocil, Amphotec) is a polyene antifungal drug, often used intravenously for systemic fungal infections. It was originally extracted from Streptomyces nodosus, a filamentous bacterium, in 1955 at the Squibb Institute for Medical Research from cultures of an undescribed streptomycete isolated from the soil collected in the Orinoco River region of Venezuela. Its name originates from the chemical's amphoteric properties. Two amphotericins, amphotericin A and amphotericin B are known, but only B is used clinically, because it is significantly more active in vivo. Amphotericin A is almost identical to amphotericin B (having a double C=C bond between the 27th and 28th carbons), but has little antifungal activity.

Currently, the drug is available as plain amphotericin B, as a cholesteryl sulfate complex (ABCD), as a lipid complex (ABLC), and as a liposomal formulation (LAmB). The latter formulations have been developed to improve tolerability for the patient, but may show considerably different pharmacokinetic characteristics compared to plain amphotericin B.

Biosynthesis[edit]

The natural route to synthesis includes polyketide synthase components.^[1]

Uses[edit]

Antifungal[edit]

Oral preparations of amphotericin B are used to treat thrush; these are virtually nontoxic, in contrast to typical intravenous therapy (IV) doses.

One of the main intravenous uses is in treating various systemic fungal infections (e.g., in critically ill, comorbidly infected or immunocompromised patients), including cryptococcal meningitis.

Amphotericin B is also commonly used in tissue culture to prevent fungi from contaminating cell cultures. It is usually sold in a concentrated solution, either on its own or in combination with the antibiotics penicillin and streptomycin.

Antiprotozoan[edit]

Another IV use is as a drug of last resort in otherwise-untreatable parasitic protozoan infections such as visceral leishmaniasis^[2]^[3] and primary amoebic meningoencephalitis.

Mechanism of action[edit]

As with other polyene antifungals, amphotericin B binds with ergosterol, a component of fungal cell membranes, forming a transmembrane channel that leads to monovalent ion (K⁺, Na⁺, H⁺ and Cl⁻) leakage, which is the primary effect leading to fungal cell death. Recently, however, researchers found evidence that pore formation is not necessarily linked to cell death^[4]^[5] The actual mechanism of action may be more complex and multifaceted.

Mechanism of toxicity[edit]

Mammalian and fungal membranes both contain sterols, a primary membrane target for amphotericin B. Because mammalian and fungal membranes are similar in structure and composition, this is one mechanism by which amphotericin B causes cellular toxicity. Amphotericin B molecules can form pores in the host membrane as well as the fungal membrane. This impairment in membrane barrier function can have lethal effects.^[5]^[6]^[7] Bacteria are not affected as their cell membrane does not contain sterols.

Amphotericin administration is limited by infusion-related toxicity. This is thought to result from innate immune production of proinflammatory cytokines.^[6]^[8]

Side-effects[edit]

Amphotericin B is well known for its severe and potentially lethal side-effects. Very often, a serious acute reaction after the infusion (1 to 3 hours later) is noted, consisting of high fever, shaking chills, hypotension, anorexia, nausea, vomiting, headache, dyspnea and tachypnea, drowsiness, and generalized weakness. This reaction sometimes subsides with later applications of the drug, and may in part be due to histamine liberation. An increase in prostaglandin synthesis may also play a role. This nearly universal febrile response necessitates a critical (and diagnostically difficult) professional determination as to whether the onset of high fever is a novel symptom of a fast-progressing disease, or merely the induced effect of the drug. To decrease the likelihood and severity of the symptoms, initial doses should be low, and increased slowly. Paracetamol, pethidine, diphenhydramine, and hydrocortisone have all been used to treat or prevent the syndrome, but the prophylactic use of these drugs is often limited by the patient's condition.

Intravenously administered amphotericin B has also been associated with multiple organ damage in therapeutic doses. Nephrotoxicity (kidney damage) is a frequently reported side-effect, and can be severe and/or irreversible. It is much milder when delivered via liposomes (AmBisome), and this is, therefore, the preferred method (see below). The integrity of the liposome is disrupted when it binds to the fungal cell wall, but is not affected by the mammalian cell membrane, thus less toxicity is seen.^[9] The association with liposomes decreases the exposure of the kidneys to amphotericin B, which explains less nephrotoxic effects.^[10] In addition, electrolyte imbalances (e.g., hypokalemia and hypomagnesemia) may also result. In the liver, increased liver enzymes and hepatotoxicity (up to and including fulminant liver failure) are common. In the circulatory system, several forms of anemia and other blood dyscrasias (leukopenia, thrombopenia), serious cardiac arrhythmias (including ventricular fibrillation), and even frank cardiac failure have been reported. Skin reactions, including serious forms, are also possible.

Interactions[edit]

Flucytosine: Toxicity of flucytosine is increased and allows a lower dose of amphotericin B. Amphotericin B may also facilitate entry of flucystosine into the fungal cell by interfering with the permeability of the fungal cell membrane.
Diuretics or cisplatin: Increased renal toxicity and increased risk of hypokalemia
Corticosteroids: Increased risk of hypokalemia
Cytostatic drugs: Increased risk of kidney damage, hypotension and bronchospasms
Other nephrotoxic drugs (like Aminoglycosides) : Increased risk of serious renal damage, monitor kidney function closely
Foscarnet, ganciclovir, tenofovir, adefovir: Risk of hematological and renal side-effects of amphotericin B are increased.
Transfusion of leukocytes : Risk of pulmonal (lung) damage occurs. Space the intervals between the application of amphotericin B and the transfusion, and monitor pulmonary function.

Clinical efficacy[edit]

Liposomal amphotericin B was effective as empirical therapy or as treatment for confirmed invasive fungal infections in several randomized, double-blind trials (n = 73 − 1095) in adult and pediatric patients.^[11]

Liposomal and lipid complex preparations[edit]

From studies, it appears that liposomal amphotericin B preparations exhibit fewer side-effects, while having similar efficacy. Various preparations have recently been introduced. All of these are more expensive than plain amphotericin B.

AmBisome is a liposomal formulation of amphotericin B for injection, developed by NeXstar Pharmaceuticals (acquired by Gilead Sciences in 1999). It is marketed by Gilead in Europe and licensed to Astellas Pharma (formerly Fujisawa Pharmaceuticals) for marketing in the USA, and Sumitomo Pharmaceuticals in Japan.

Fungisome is a liposomal complex of amphotericin B, and being the latest and cheapest addition to the lipid formulations of amphotericin B, it has many advantages. It is marketed by Lifecare Innovations of India. Other formulations include Amphotec (Intermune) and Abelcet (Sigma-Tau Pharmaceuticals). Abelcet is not a liposomal preparation but rather a lipid complex preparation.

Oral preparations[edit]

A major barrier to the use of amphotericin in resource-poor settings is that it must be given intravenously (except for topical applications). An oral preparation exists, but is not yet commercially available.^[12] The amphipathic nature of amphotericin along with its low solubility and permeability has posed major hurdles for oral administration. However recently novel nanoparticulate drug delivery systems such as AmbiOnp,^[13] Nanosuspensions, Lipid based drug delivery systems including Cochleates, Self-emulsifying drug delivery systems (SEDDS),^[14] Solid lipid nanoparticles (SLNs)^[15] and Polymeric Nanoparticles^[16] have demonstrated great potential for oral formulation of amphotericin B.^[17]

References[edit]

^ Khan N, Rawlings B, Caffrey P (2011-01-26). "A labile point in mutant amphotericin polyketide synthases". Biotechnol Lett. 33 (6): 1121–6. doi:10.1007/s10529-011-0538-3. PMID 21267757.
^ Kafetzis DA, Velissariou IM, Stabouli S, Mavrikou M, Delis D, Liapi G (January 2005). "Treatment of paediatric visceral leishmaniasis: amphotericin B or pentavalent antimony compounds?". Int. J. Antimicrob. Agents 25 (1): 26–30. doi:10.1016/j.ijantimicag.2004.09.011. PMID 15620822.
^ Veerareddy PR, Vobalaboina V, Ali N (December 2008). "Antileishmanial activity, pharmacokinetics and tissue distribution studies of mannose-grafted amphotericin B lipid nanospheres". J Drug Target 17 (2): 140–7. doi:10.1080/10611860802528833. PMID 19089691.
^ Angewandte Chemie Int. Ed. Engl. 2004^{[page needed]}
^ ^a ^b Baginski, M.; Czub, J. (2009). "Amphotericin B and Its New Derivatives–Mode of Action". Current Drug Metabolism 10 (5): 459–69. PMID 19689243.
^ ^a ^b Laniado-Laborin R. and Cabrales-Vargas MN. Amphotericin B: side effects and toxicity. Revista Iberoamericana de Micologia. (2009): 223–7.
^ Pfizer. Amphocin. Accessed at http://www.pfizer.com/files/products/uspi_amphocin.pdf on Feb 18 2010.
^ Drew, R. Pharmacology of amphotericin B. Uptodate. Sep 2009. Accessed at http://www.utdol.com/online/content/topic.do?topicKey=antibiot/4619&selectedTitle=2~150&source=search_result on Feb 18 2010.
^ Jill Adler-Moore,* and Richard T. liposomal formulation, structure, mechanism of action and pre-clinical experience. Journal of Antimicrobial Chemotherapy (2002) 49, 21–30
^ J. Czumb, M. Baginksi. Amphotericin B and Its New Derivatives Mode of action. Department of pharmaceutical Technology and Biochemistry. Faculty of Chemistry, Gdnsk University of Technology. 2009, 10-459-469.
^ Moen M,Lyseng-Wialliamson KA, Scott LJ.[1].Drugs 2009;69(3):361–392. doi:10.2165/00003495-200969030-00010.
^ Wasan KM, Wasan EK, Gershkovich P, et al. (2009). "Highly Effective oral amphotericin B formulation against murine visceral leishmaniasis". J Infect Dis 200 (3): 357–360. doi:10.1086/600105. PMID 19545212.
^ Patel, Pratikkumar A., and Vandana B. Patravale. "AmbiOnp: solid lipid nanoparticles of amphotericin B for oral administration." Journal of Biomedical Nanotechnology 7.5 (2011): 632-639.
^ Wasan EK, Bartlett K, Gershkovich P, Sivak O, Banno B, Wong Z, Gagnon J, Gates B, Leon CG, Wasan KM. Development and characterization of oral lipid-based amphotericin B formulations with enhanced drug solubility, stability and antifungal activity in rats infected with Aspergillus fumigatus or Candida albicans. International Journal of Pharmaceutics. 2009; 372(1-2):76-84
^ Patel PA, Patravale,VB. AmbiOnp: solid lipid nanoparticles of amphotericin B for oral administration. Journal of Biomedical Nanotechnology.2011; 7(5):632-639
^ Italia JL, Yahya MM, Singh D. Biodegradable nanoparticles improve oral Bioavailability of Amphotericin B and Show Reduced Nephrotoxicity Compared to Intravenous Fungizone®. Pharmaceutical Research. 2009; 26 (6): 1324 -1331
^ Patel PA, Fernandes CB, Pol AS, Patravale VB. Oral Amphotericin B: Challenges and avenues. Int. J. Pharm. Biosci. Technol. 2013;1(1):1–9

External links[edit]

AmBisome web site run by Astella Pharma
"Special issue". Journal of Postgraduate Medicine 51 (Suppl). 2005.
Review Article: Oral Amphotericin B:Challenges and avenues

UpToDate Contents

全文を閲覧するには購読必要です。 To read the full text you will need to subscribe.

1. アムホテシリンBによる腎毒性 amphotericin b nephrotoxicity
2. アムホテリシンBの薬理 pharmacology of amphotericin b
3. 小児におけるカンジダ血症の治療 treatment of candidemia in children
4. 新生児におけるカンジダ感染の治療 treatment of candida infection in neonates
5. 新生児における特殊な真菌感染症 unusual fungal infections in the neonate

English Journal

Differential internalization of amphotericin B - Conjugated nanoparticles in human cells and the expression of heat shock protein 70.

Paulo CS, Lino MM, Matos AA, Ferreira LS.SourceCNC-Center for Neurosciences and Cell Biology, University of Coimbra, 3004-517 Coimbra, Portugal; Biocant, Biotechnology Innovation Center, 3060-197 Cantanhede, Portugal.
Biomaterials.Biomaterials.2013 Jul;34(21):5281-93. doi: 10.1016/j.biomaterials.2013.03.048. Epub 2013 Apr 8.
Although a variety of nanoparticles (NPs) functionalized with amphotericin B, an antifungal agent widely used in the clinic, have been studied in the last years their cytotoxicity profile remains elusive. Here we show that human endothelial cells take up high amounts of silica nanoparticles (SNPs) c
PMID 23578560

Lipid-based microtubes for topical delivery of amphotericin B.

Salerno C, Chiappetta DA, Arechavala A, Gorzalczany S, Scioscia SL, Bregni C.SourceDepartment of Pharmaceutical Technology, Faculty of Pharmacy and Biochemistry, University of Buenos Aires. Buenos Aires, Argentina. salernoclaudia@hotmail.com
Colloids and surfaces. B, Biointerfaces.Colloids Surf B Biointerfaces.2013 Jul 1;107:160-6. doi: 10.1016/j.colsurfb.2013.02.001. Epub 2013 Feb 13.
The self-assembly process is a valuable tool for constructing nano and microstructures. Microtubes (MTs) self-assembled from amphiphiles are novel promising nanomaterials as they have easy self-assembly in aqueous solutions, reproducibility and biocompatibility. The incorporation of amphotericin B (
PMID 23500726

Spray dried chitosan-EDTA superior microparticles as solid substrate for the oral delivery of amphotericin B.

Singh K, Tiwary AK, Rana V.SourcePharmaceutics Division, Department of Pharmaceutical Sciences and Drug Research, Punjabi University, Patiala 147002, India.
International journal of biological macromolecules.Int J Biol Macromol.2013 Jul;58:310-9. doi: 10.1016/j.ijbiomac.2013.04.053. Epub 2013 Apr 23.
The present investigation was aimed at synthesis of chitosan-EDTA superior microparticles (COECH) bearing high oil adsorbing and oil desorbing properties. These superior particles were prepared by thermal amide conjugation of COO(-) group of EDTA with NH2 group of chitosan employing spray-drying tec
PMID 23624284

Japanese Journal

Physiology : Amphotericin B Induces Glial Cell Line-Derived Neurotrophic Factor in the Rat Brain

MOTOYOSHI-YAMASHIRO Akiko,TAKANO Katsura,KAWABE Kenji [他]
The journal of veterinary medical science 76(10), 1353-1358, 2014-10
NAID 40020245217

造血器疾患とムーコル症

渡辺哲,亀井克彦
血液内科 69(4), 584-588, 2014-10
NAID 40020237146

In-Vitro Evaluation of the Anti-Leishmanial Activity of Euphorbia Helioscopia Stem Extract In Comparison With Synthetic Drug Amphotericin B

Qureshi Naveeda Akhtar,Rahman Hamid Ur,Ali Abid [他]
Asian journal of natural and applied sciences 3(3), 12-17, 2014-09
NAID 40020223836

「アンホテリシン」

Amphotericin B
Systematic (IUPAC) name
	(1R,3S,5R,6R,9R, 11R,15S,16R,17R,18S,19E,21E, 23E,25E,27E,29E,31E,33R,35S,36R,37S)- 33-[(3-amino- 3,6-dideoxy- β-D-mannopyranosyl)oxy]- 1,3,5,6,9,11,17,37-octahydroxy- 15,16,18-trimethyl- 13-oxo- 14,39-dioxabicyclo [33.3.1] nonatriaconta- 19,21,23,25,27,29,31-heptaene- 36-carboxylic acid
Clinical data
Trade names	Fungizone
AHFS/Drugs.com	monograph
Pregnancy cat.	B (US)
Legal status	Rx-only, hospitalization recommended.
Routes	I.V. (slow infusion only)
Pharmacokinetic data
Bioavailability	100% (IV)
Metabolism	renal
Half-life	initial phase : 24 hours,; second phase : approx. 15 days
Excretion	40% found in urine after single cumulated over several days; biliar excretion also important
Identifiers
CAS number	1397-89-3
ATC code	A01AB04 A07AA07, G01AA03, J02AA01
PubChem	CID 14956
DrugBank	DB00681
ChemSpider	10237579
KEGG	D00203
ChEBI	CHEBI:2682
ChEMBL	CHEMBL267345
NIAID ChemDB	000096
Chemical data
Formula	C47H73NO17
Mol. mass	923.49
	SMILES O=C(O)[C@@H]3[C@@H](O)C[C@@]2(O)C[C@@H](O)C[C@@H](O)[C@H](O)CC[C@@H](O)C[C@@H](O)CC(=O)O[C@@H](C)[C@H](C)[C@H](O)[C@@H](C)C=CC=CC=CC=CC=CC=CC=C[C@H](O[C@@H]1O[C@H](C)[C@@H](O)[C@H](N)[C@@H]1O)C[C@@H]3O2;
	InChI InChI=1S/C47H73NO17/c1-27-17-15-13-11-9-7-5-6-8-10-12-14-16-18-34(64-46-44(58)41(48)43(57)30(4)63-46)24-38-40(45(59)60)37(54)26-47(61,65-38)25-33(51)22-36(53)35(52)20-19-31(49)21-32(50)23-39(55)62-29(3)28(2)42(27)56/h5-18,27-38,40-44,46,49-54,56-58,61H,19-26,48H2,1-4H3,(H,59,60)/b6-5+,9-7+,10-8+,13-11+,14-12+,17-15+,18-16+/t27-,28-,29-,30+,31+,32+,33-,34-,35+,36+,37-,38-,40+,41-,42+,43+,44-,46-,47+/m0/s1 ; Key:APKFDSVGJQXUKY-INPOYWNPSA-N ;
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