Crohn's disease
Classification and external resources
The three most common sites of intestinal involvement in Crohn's disease are ileal, ileocolic and colonic.[1]
ICD-10	K50
ICD-9	555
OMIM	266600
DiseasesDB	3178
MedlinePlus	000249
eMedicine	med/477 ped/507 radio/197
MeSH	D003424

Crohn's disease, also known as Crohn syndrome and regional enteritis, is a type of inflammatory bowel disease that may affect any part of the gastrointestinal tract from mouth to anus, causing a wide variety of symptoms. It primarily causes abdominal pain, diarrhea (which may be bloody if inflammation is severe), vomiting, or weight loss,^[1][2][3] but may also cause complications outside the gastrointestinal tract such as anemia, skin rashes, arthritis, inflammation of the eye, tiredness, and lack of concentration.^[1] Crohn's disease is caused by interactions between environmental, immunological and bacterial factors in genetically susceptible individuals.^[4][5][6] This results in a chronic inflammatory disorder, in which the body's immune system attacks the gastrointestinal tract possibly directed at microbial antigens.^[5][7] While Crohn's is an immune related disease, it does not appear to be an autoimmune disease (in that the immune system is not being triggered by the body itself).^[8] The exact underlying immune problem is not clear; however it may be an immune deficiency state.^[7][9][10]

There is a genetic association with Crohn's disease, primarily with variations of the NOD2 gene and its protein, which senses bacterial cell walls. Siblings of affected individuals are at higher risk.^[11] Males and females are equally affected. Tobacco smokers are two times more likely to develop Crohn's disease than nonsmokers.^[12] Crohn's disease affects between 400,000 and 600,000 people in North America.^[13] Prevalence estimates for Northern Europe have ranged from 27–48 per 100,000.^[14] Crohn's disease tends to present initially in the teens and twenties, with another peak incidence in the fifties to seventies, although the disease can occur at any age.^[1][15] There is no known pharmaceutical or surgical cure for Crohn's disease. Treatment options are restricted to controlling symptoms, maintaining remission, and preventing relapse. The disease was named after gastroenterologist Burrill Bernard Crohn, who, in 1932, together with two other colleagues at Mount Sinai Hospital in New York, described a series of patients with inflammation of the terminal ileum, the area most commonly affected by the illness.^[16]

Signs and symptoms

Signs and symptoms

[ v t e ]	Crohn's disease	Ulcerative colitis
Defecation	Often porridge-like[17], sometimes steatorrhea	Often mucus-like and with blood[17]
Tenesmus	Less common[17]	More common[17]
Fever	Common[17]	Indicates severe disease[17]
Fistulae	Common[18]	Seldom
Weight loss	Often	More seldom

Gastrointestinal

Many people with Crohn's disease have symptoms for years prior to the diagnosis.^[19] The usual onset is between 15 and 30 years of age, but can occur at any age.^[20] Because of the 'patchy' nature of the gastrointestinal disease and the depth of tissue involvement, initial symptoms can be more subtle than those of ulcerative colitis. People with Crohn's disease experience chronic recurring periods of flare-ups and remission.^[21]

Abdominal pain may be the initial symptom of Crohn's disease. It is often accompanied by diarrhea, especially in those who have had surgery. The diarrhea may or may not be bloody. The nature of the diarrhea in Crohn's disease depends on the part of the small intestine or colon involved. Ileitis typically results in large-volume, watery feces. Colitis may result in a smaller volume of feces of higher frequency. Fecal consistency may range from solid to watery. In severe cases, an individual may have more than 20 bowel movements per day and may need to awaken at night to defecate.^{[1][15][22][23]} Visible bleeding in the feces is less common in Crohn's disease than in ulcerative colitis, but may be seen in the setting of Crohn's colitis.^[1] Bloody bowel movements are typically intermittent, and may be bright or dark red in color. In the setting of severe Crohn's colitis, bleeding may be copious.^[15] Flatulence and bloating may also add to the intestinal discomfort.^[15]

Symptoms caused by intestinal stenosis are also common in Crohn's disease. Abdominal pain is often most severe in areas of the bowel with stenoses. Persistent vomiting and nausea may indicate stenosis from small bowel obstruction or disease involving the stomach, pylorus or duodenum.^[15] Although the association is greater in the context of ulcerative colitis, Crohn's disease may also be associated with primary sclerosing cholangitis, a type of inflammation of the bile ducts.^[24]

Perianal discomfort may also be prominent in Crohn's disease. Itchiness or pain around the anus may be suggestive of inflammation, fistulization or abscess around the anal area^[1] or anal fissure. Perianal skin tags are also common in Crohn's disease.^[25] Fecal incontinence may accompany perianal Crohn's disease. At the opposite end of the gastrointestinal tract, the mouth may be affected by non-healing sores (aphthous ulcers). Rarely, the esophagus, and stomach may be involved in Crohn's disease. These can cause symptoms including difficulty swallowing (dysphagia), upper abdominal pain, and vomiting.^[26]

Systemic

Crohn's disease, like many other chronic, inflammatory diseases, can cause a variety of systemic symptoms.^[1] Among children, growth failure is common. Many children are first diagnosed with Crohn's disease based on inability to maintain growth.^[27] As it may manifest at the time of the growth spurt in puberty, up to 30% of children with Crohn's disease may have retardation of growth.^[28] Fever may also be present, though fevers greater than 38.5 ˚C (101.3 ˚F) are uncommon unless there is a complication such as an abscess.^[1] Among older individuals, Crohn's disease may manifest as weight loss, usually related to decreased food intake, since individuals with intestinal symptoms from Crohn's disease often feel better when they do not eat and might lose their appetite.^[27] People with extensive small intestine disease may also have malabsorption of carbohydrates or lipids, which can further exacerbate weight loss.^[29]

Extraintestinal

In addition to systemic and gastrointestinal involvement, Crohn's disease can affect many other organ systems.^[30] Inflammation of the interior portion of the eye, known as uveitis, can cause eye pain, especially when exposed to light (photophobia). Inflammation may also involve the white part of the eye (sclera), a condition called episcleritis. Both episcleritis and uveitis can lead to loss of vision if untreated.

Crohn's disease that affects the ileum may result in an increased risk for gallstones. This is due to a decrease in bile acid resorption in the ileum and the bile gets excreted in the stool. As a result, the cholesterol/bile ratio increases in the gallbladder, resulting in an increased risk for gallstones.^[31]

Crohn's disease is associated with a type of rheumatologic disease known as seronegative spondyloarthropathy. This group of diseases is characterized by inflammation of one or more joints (arthritis) or muscle insertions (enthesitis). The arthritis can affect larger joints, such as the knee or shoulder, or may exclusively involve the small joints of the hands and feet. The arthritis may also involve the spine, leading to ankylosing spondylitis if the entire spine is involved or simply sacroiliitis if only the lower spine is involved. The symptoms of arthritis include painful, warm, swollen, stiff joints and loss of joint mobility or function.^[21]

Crohn's disease may also involve the skin, blood, and endocrine system. One type of skin manifestation, erythema nodosum, presents as red nodules usually appearing on the shins. Erythema nodosum is due to inflammation of the underlying subcutaneous tissue, and is characterized by septal panniculitis. Another skin lesion, pyoderma gangrenosum, is typically a painful ulcerating nodule. Crohn's disease also increases the risk of blood clots; painful swelling of the lower legs can be a sign of deep venous thrombosis, while difficulty breathing may be a result of pulmonary embolism. Autoimmune hemolytic anemia, a condition in which the immune system attacks the red blood cells, is also more common in Crohn's disease and may cause fatigue, pallor, and other symptoms common in anemia. Clubbing, a deformity of the ends of the fingers, may also be a result of Crohn's disease. Finally, Crohn's disease may cause osteoporosis, or thinning of the bones. Individuals with osteoporosis are at increased risk of bone fractures.^[14]

People with Crohn's disease often have anemia, due to B12, folate, or iron deficiency. The most common is iron deficiency anemia from chronic blood loss, but also persistent inflammation leading to increased hepcidin levels, restricting iron absorption in the duodenum. As Crohn's disease most commonly affects the terminal ileum where the vtamin B12/intrinsic factor complex is absorbed, B12 deficiency is often seen. This is particularly common after surgery to remove the ileum. Involvement of the duodenum and jejunum can impair the absorption of many other nutrients including folate. If Crohn's disease affects the stomach, production of intrinsic factor can be reduced.

Crohn's disease can also cause neurological complications (reportedly in up to 15%).^[32] The most common of these are seizures, stroke, myopathy, peripheral neuropathy, headache and depression.^[32]

People with Crohn's often also have issues with small bowel bacterial overgrowth syndrome, which has similar symptoms.^[33]

In the oral cavity people with crohn's may develop cheilitis granulomatosa and other forms of orofacial granulomatosis, pyostomatitis vegetans, recurrent aphthous stomatitis, geographic tongue and migratory stomatitis in higher prevalence than the general population.^[34]

Cause

Risk factors

[ v t e ]	Crohn's disease	Ulcerative colitis
Smoking	Higher risk for smokers	Lower risk for smokers[35]
Age	Usual onset between 15 and 30 years[36]	Peak incidence between 15 and 25 years

Crohn's disease seems to be caused by a combination of environmental factors and genetic predisposition.^[37] Crohn's is the first genetically complex disease in which the relationship between genetic risk factors and the immune system is understood in considerable detail.^[38] Each individual risk mutation makes a small contribution to the overall risk of Crohn's (approximately 1:200). The genetic data, and direct assessment of peoples immunity, indicates a malfunction in the innate immune system.^[39] In this view, the chronic inflammation of Crohn's is caused when the adaptive immune system tries to compensate for a deficient innate immune system.^[40]

Genetics

Crohn's has a genetic component.^[41] Because of this, siblings of known people with Crohn's are 30 times more likely to develop Crohn's than the general population.

The first mutation found to be associated with Crohn's was a frameshift in the NOD2 gene (also known as the CARD15 gene),^[42] followed by the discovery of point mutations.^[43] By now, over thirty genes have been associated. A biological function is known for most of them. For example, one association is with mutations in the XBP1 gene, which is involved in the unfolded protein response pathway of the endoplasmatic reticulum.^[44][45] There is considerable overlap between susceptibility loci for IBD and mycobacterial infections.^[46]

Immune system

There was a prevailing view that Crohn's disease is a primary T cell autoimmune disorder, however a newer theory hypothesizes that Crohn's results from an impaired innate immunity.^[47] The later hypothesis describes impaired cytokine secretion by macrophages, which contributes to impaired innate immunity and leads to a sustained microbial-induced inflammatory response in the colon, where the bacterial load is high.^[5][39] Another theory is that the inflammation of Crohn's was caused by an overactive T_h1 cytokine response.^[48] More recent^[when?] studies argue that T_h17 is more important.^[49]

The most recent (2007) gene to be implicated in Crohn's disease is ATG16L1, which may induce autophagy and hinder the body's ability to attack invasive bacteria.^[50] Another recent study has theorized that the human immune system traditionally evolved with the presence of parasites inside the body, and that the lack thereof due to modern hygiene standards has weakened the immune system. Test subjects were reintroduced to harmless parasites, with positive response.^[51]

Microbes

Current thinking is that microorganisms are taking advantage of their host's weakened mucosal layer and inability to clear bacteria from the intestinal walls, which are both symptoms of Crohn's.^[52] Different strains found in tissue and different outcomes to antibiotics therapy and resistance suggest Crohn's Disease is not one disease, but an umbrella of diseases related to different pathogens.^[53][54]

Some studies have suggested a role for Mycobacterium avium subspecies paratuberculosis (MAP), which causes a similar disease, Johne's disease, in cattle.^[55] NOD2, a gene involved in Crohn’s genetic susceptibility, is associated with diminished killing of MAP by macrophages, reduced innate and adaptive immunity in the host and impaired immune responses required for control of intracellular mycobacterial infection.^[56][57] Macrophages infected with viable MAP are associated with high production of TNF-α.^[58][59]

Other studies have linked specific strains of enteroadherent E. coli to the disease.^[60] Adherent-invasive Escherichia coli (AIEC), are more common in people with CD,^[61][62][63] have the ability to make strong biofilms compared to non-AIEC strains correlating with high adhesion and invasion indices^[64][65] of neutrophils and the ability to block autophagy at the autolysosomal step, which allows for intracellular survival of the bacteria and induction of inflammation.^[66] Inflammation drives the proliferation of AIEC and dysbiosis in the ileum, irrespective of genotype.^[67] AIEC strains replicate extensively into macrophages inducing the secretion of very large amounts of TNF-α.^[68]

Mouse studies have suggested some symptoms of Crohn's disease, ulcerative colitis and irritable bowel syndrome have the same underlying cause. Biopsy samples taken from the colons of all three patient groups were found to produce elevated levels of a serine protease.^[69] Experimental introduction of the serine protease into mice has been found to produce widespread pain associated with irritable bowel syndrome, as well as colitis, which is associated with all three diseases.^[70] Regional and temporal variations in those illnesses follow those associated with infection with the protozoan Blastocystis.^[71]

The "cold-chain" hypothesis is that psychrotrophic bacteria such as Yersinia and Listeria species contribute to the disease. A statistical correlation was found between the advent of the use of refrigeration in the United States and various parts of Europe and the rise of the disease.^[72][73][74]

There is an apparent connection between Crohn's disease, Mycobacterium, other pathogenic bacteria, and genetic markers.^[75][76] In many individuals, genetic factors predispose individuals to Mycobacterium avium subsp. paratuberculosis infection. This bacterium then produces mannins, which protect both itself and various bacteria from phagocytosis, which causes a variety of secondary infections.^[77]

Still, this relationship between specific types of bacteria and Crohn's disease remains unclear.^[78][79]

Environmental factors

The increased incidence of Crohn's in the industrialized world indicates an environmental component. Crohn's is associated with an increased intake of animal protein, milk protein and an increased ratio of omega-6 to omega-3 polyunsaturated fatty acids.^[80] Those who consume vegetable proteins appear to have a lower incidence of Crohn's disease. Consumption of fish protein has no association.^[80] Smoking increases the risk of the return of active disease (flares).^[12] The introduction of hormonal contraception in the United States in the 1960s is associated with a dramatic increase in incidence, and one hypothesis is that these drugs work on the digestive system in ways similar to smoking.^[81] Isotretinoin is associated with Crohn's.^[82][83][84] Although stress is sometimes claimed to exacerbate Crohn's disease, there is no concrete evidence to support such claim.^[85] Dietary microparticles, such as those found in toothpaste, have been studied as they produce effects on immunity, but they were not consumed in greater amounts in patients with Crohn's.^[86][87]

Pathophysiology

Pathophysiology

[ v t e ]	Crohn's disease	Ulcerative colitis
Cytokine response	Associated with Th17[49]	Vaguely associated with Th2

During a colonoscopy, biopsies of the colon are often taken to confirm the diagnosis. Certain characteristic features of the pathology seen point toward Crohn's disease; it shows a transmural pattern of inflammation, meaning the inflammation may span the entire depth of the intestinal wall.^[1] Ulceration is an outcome seen in highly active disease. There is usually an abrupt transition between unaffected tissue and the ulcer - a characteristic sign known as skip lesions. Under a microscope, biopsies of the affected colon may show mucosal inflammation, characterized by focal infiltration of neutrophils, a type of inflammatory cell, into the epithelium. This typically occurs in the area overlying lymphoid aggregates. These neutrophils, along with mononuclear cells, may infiltrate the crypts, leading to inflammation (crypititis) or abscess (crypt abscess). Granulomas, aggregates of macrophage derivatives known as giant cells, are found in 50% of cases and are most specific for Crohn's disease. The granulomas of Crohn's disease do not show "caseation", a cheese-like appearance on microscopic examination characteristic of granulomas associated with infections, such as tuberculosis. Biopsies may also show chronic mucosal damage, as evidenced by blunting of the intestinal villi, atypical branching of the crypts, and a change in the tissue type (metaplasia). One example of such metaplasia, Paneth cell metaplasia, involves development of Paneth cells (typically found in the small intestine and a key regulator of intestinal microbiota) in other parts of the gastrointestinal system.^[88][89]

Diagnosis

The diagnosis of Crohn's disease can sometimes be challenging,^[19] and a number of tests are often required to assist the physician in making the diagnosis.^[15] Even with a full battery of tests, it may not be possible to diagnose Crohn's with complete certainty; a colonoscopy is approximately 70% effective in diagnosing the disease, with further tests being less effective. Disease in the small bowel is particularly difficult to diagnose, as a traditional colonoscopy allows access to only the colon and lower portions of the small intestines; introduction of the capsule endoscopy^[90] aids in endoscopic diagnosis. Multinucleated giant cells, a common finding in the lesions of Crohn's disease, are less common in the lesions of lichen nitidus.^[91]

• Endoscopic image of Crohn's colitis showing deep ulceration

• CT scan showing Crohn's disease in the fundus of the stomach

• This endoscopic image of Crohn's colitis showing diffuse loss of mucosal architecture, friability and exudate

• Endoscopic biopsy showing granulomatous inflammation of the colon in a case of Crohn's disease.

• Section of colectomy showing transmural inflammation

Classification

Crohn's disease is one type of inflammatory bowel disease (IBD). It typically manifests in the gastrointestinal tract and can be categorized by the specific tract region affected. A disease of both the ileum (the last part of the small intestine that connects to the large intestine), and the large intestine, Ileocolic Crohn's accounts for fifty percent of cases. Crohn's ileitis, manifest in the ileum only, accounts for thirty percent of cases, while Crohn's colitis, of the large intestine, accounts for the remaining twenty percent of cases and may be particularly difficult to distinguish from ulcerative colitis. Gastroduodenal Crohn's disease causes inflammation in the stomach and first part of the small intestine, called the duodenum. Jejunoileitis causes spotty patches of inflammation in the top half of the small intestine, called the jejunum (MedlinePlus 2010). The disease can attack any part of the digestive tract, from mouth to anus. However, individuals affected by the disease rarely fall outside these three classifications, with presentations in other areas.^[1]

Crohn's disease may also be categorized by the behavior of disease as it progresses. These categorizations formalized in the Vienna classification of the disease.^[92] There are three categories of disease presentation in Crohn's disease: stricturing, penetrating, and inflammatory. Stricturing disease causes narrowing of the bowel that may lead to bowel obstruction or changes in the caliber of the feces. Penetrating disease creates abnormal passageways (fistulae) between the bowel and other structures, such as the skin. Inflammatory disease (or nonstricturing, nonpenetrating disease) causes inflammation without causing strictures or fistulae.^[92][93]

Endoscopy

A colonoscopy is the best test for making the diagnosis of Crohn's disease, as it allows direct visualization of the colon and the terminal ileum, identifying the pattern of disease involvement. On occasion, the colonoscope can travel past the terminal ileum, but it varies from person to person. During the procedure, the gastroenterologist can also perform a biopsy, taking small samples of tissue for laboratory analysis, which may help confirm a diagnosis. As 30% of Crohn's disease involves only the ileum,^[1] cannulation of the terminal ileum is required in making the diagnosis. Finding a patchy distribution of disease, with involvement of the colon or ileum, but not the rectum, is suggestive of Crohn's disease, as are other endoscopic stigmata.^[94] The utility of capsule endoscopy for this, however, is still uncertain.^[95] A "cobblestone"-like appearance is seen in approximately 40% of cases of Crohn's disease upon colonoscopy, representing areas of ulceration separated by narrow areas of healthy tissue.

Radiologic tests

A small bowel follow-through may suggest the diagnosis of Crohn's disease and is useful when the disease involves only the small intestine. Because colonoscopy and gastroscopy allow direct visualization of only the terminal ileum and beginning of the duodenum, they cannot be used to evaluate the remainder of the small intestine. As a result, a barium follow-through X-ray, wherein barium sulfate suspension is ingested and fluoroscopic images of the bowel are taken over time, is useful for looking for inflammation and narrowing of the small bowel.^[94][96] Barium enemas, in which barium is inserted into the rectum and fluoroscopy is used to image the bowel, are rarely used in the work-up of Crohn's disease due to the advent of colonoscopy. They remain useful for identifying anatomical abnormalities when strictures of the colon are too small for a colonoscope to pass through, or in the detection of colonic fistulae (in this case contrast should be performed with iodate substances).^[97]

CT and MRI scans are useful for evaluating the small bowel with enteroclysis protocols.^[98] They are also useful for looking for intra-abdominal complications of Crohn's disease, such as abscesses, small bowel obstructions, or fistulae.^[99] Magnetic resonance imaging (MRI) is another option for imaging the small bowel as well as looking for complications, though it is more expensive and less readily available^[100]

Blood tests

A complete blood count may reveal anemia, which commonly is caused by blood loss leading to iron deficiency (a microcytic anemia) or by vitamin B₁₂ deficiency (a macrocytic anemia), usually caused by ileal disease impairing vitamin B₁₂ absorption. Rarely autoimmune hemolysis may occur.^[101] Ferritin levels help assess if iron deficiency is contributing to the anemia. Erythrocyte sedimentation rate (ESR) and C-reactive protein help assess the degree of inflammation, which is important as ferritin can also be raised in inflammation.^[102] Serum iron, total iron binding capacity and transferrin saturation may be more easily interpreted in inflammation. Anemia of chronic disease results in a normocytic anemia. Other causes of anemia include medication used in treatment of inflammatory bowel disease, like azathioprine, which can lead to cytopenia, and sulfasalazine, which can also result in folate deficiency. Testing for Saccharomyces cerevisiae antibodies (ASCA) and antineutrophil cytoplasmic antibodies (ANCA) has been evaluated to identify inflammatory diseases of the intestine^[103] and to differentiate Crohn's disease from ulcerative colitis.^[104] Furthermore, increasing amounts and levels of serological antibodies such as ASCA, antilaminaribioside [Glc(β1,3)Glb(β); ALCA], antichitobioside (GlcNAc(β1,4)GlcNAc(β); ACCA], antimannobioside [Man(α1,3)Man(α)AMCA], antiLaminarin [Glc(β1,3))3n(Glc(β1,6))n; anti-L] and antichitin [(GlcNAc(β1,4)n; anti-C] associate with disease behavior and surgery, and may aid in the prognosis of Crohn's disease.^{[105][106][107][108]}

Comparison with ulcerative colitis

The most common disease that mimics the symptoms of Crohn's disease is ulcerative colitis, as both are inflammatory bowel diseases that can affect the colon with similar symptoms. It is important to differentiate these diseases, since the course of the diseases and treatments may be different. In some cases, however, it may not be possible to tell the difference, in which case the disease is classified as indeterminate colitis.^[1][15][22]

Diagnostic findings

Sign [ v t e ]	Crohn's disease	Ulcerative colitis
Terminal ileum involvement	Commonly	Seldom
Colon involvement	Usually	Always
Rectum involvement	Seldom	Usually[35]
Involvement around the anus	Common[18]	Seldom
Bile duct involvement	No increase in rate of primary sclerosing cholangitis	Higher rate[109]
Distribution of Disease	Patchy areas of inflammation (Skip lesions)	Continuous area of inflammation[35]
Endoscopy	Deep geographic and serpiginous (snake-like) ulcers	Continuous ulcer
Depth of inflammation	May be transmural, deep into tissues[1][18]	Shallow, mucosal
Stenosis	Common	Seldom
Granulomas on biopsy	May have non-necrotizing non-peri-intestinal crypt granulomas[18][110][111]	Non-peri-intestinal crypt granulomas not seen[35]

Management

Management

[ v t e ]	Crohn's disease	Ulcerative colitis
Mesalazine	Less useful[112]	More useful[112]
Antibiotics	Effective in long-term[113]	Generally not useful[114]
Surgery	Often returns following removal of affected part	Usually cured by removal of colon

There is no cure for Crohn's disease and remission may not be possible or prolonged if achieved. In cases where remission is possible, relapse can be prevented and symptoms controlled with medication, lifestyle and dietary changes, changes to eating habits (eating smaller amounts more often), reduction of stress, moderate activity and exercise. Surgery is generally counter-indicated and has not been shown to prevent remission. Adequately controlled, Crohn's disease may not significantly restrict daily living.^[115] Treatment for Crohn's disease is only when symptoms are active and involve first treating the acute problem, then maintaining remission.

Lifestyle changes

Certain lifestyle changes can reduce symptoms, including dietary adjustments, elemental diet, proper hydration, and smoking cessation. Smoking may increase Crohn's disease; stopping is recommended. Eating small meals frequently instead of big meals may also help with a low appetite. To manage symptoms have a balanced diet with proper portion control. Fatigue can be helped with regular exercise, a healthy diet, and enough sleep. A food diary may help with identifying foods that trigger symptoms. Some people should follow a low dietary fiber diet to control symptoms especially if fibrous foods cause symptoms.^[115] Some find relief in eliminating casein (protein found in cow's milk) and gluten (protein found in wheat, rye and barley) from their diets. They may have specific dietary intolerances (not allergies).^[116]

Medication

Acute treatment uses medications to treat any infection (normally antibiotics) and to reduce inflammation (normally aminosalicylate anti-inflammatory drugs and corticosteroids). When symptoms are in remission, treatment enters maintenance, with a goal of avoiding the recurrence of symptoms. Prolonged use of corticosteroids has significant side-effects; as a result, they are, in general, not used for long-term treatment. Alternatives include aminosalicylates alone, though only a minority are able to maintain the treatment, and many require immunosuppressive drugs.^[18] It has been also suggested that antibiotics change the enteric flora, and their continuous use may pose the risk of overgrowth with pathogens such as Clostridium difficile.^[117]

Medications used to treat the symptoms of Crohn's disease include 5-aminosalicylic acid (5-ASA) formulations, prednisone, immunomodulators such as azathioprine (given as the prodrug for 6-mercaptopurine), methotrexate, infliximab, adalimumab,^[22] certolizumab^[118] and natalizumab.^[119][120] Hydrocortisone should be used in severe attacks of Crohn's disease.^[121]

The gradual loss of blood from the gastrointestinal tract, as well as chronic inflammation, often leads to anemia, and professional guidelines suggest routinely monitoring for this.^{[122][123][124]} Adequate disease control usually improves anemia of chronic disease, but iron deficiency may require treatment with iron supplements. Guidelines vary as to how iron should be administered. Some^[124] advise parenteral iron as first line as it works faster, has fewer gastrointestinal side effects, and is unaffected by inflammation reducing enteral absorption.

Other guidelines^[123] advise oral iron as first line with parenteral iron reserved for those that fail to adequately respond as oral iron is considerably cheaper. All agree that severe anemia (hemoglobin under 10g/dL) should be treated with parenteral iron. Blood transfusion should be reserved for those who are cardiovascularly unstable, due the relatively poor safety profile, lack of long term efficacy, and cost.^[123]

Surgery

Crohn's cannot be cured by surgery, though it is used in the case of partial or full blockage of the intestine. Surgery may also be required for complications such as obstructions, fistulas, or abscesses, or if the disease does not respond to drugs. After the first surgery, Crohn's usually shows up at the site of the resection, however it can appear in other locations. After a resection, scar tissue builds up, which can cause strictures, which form when the intestines become too small to allow excrement to pass through easily, which can lead to a blockage. After the first resection, another resection may be necessary within five years.^[125] For patients with an obstruction due to a stricture, two options for treatment are strictureplasty and resection of that portion of bowel. There is no statistical significance between strictureplasty alone versus strictureplasty and resection in cases of duodenal involvement. In these cases, re-operation rates were 31% and 27%, respectively, indicating that strictureplasty is a safe and effective treatment for selected people with duodenal involvement.^[126]

Short bowel syndrome (SBS, also short gut syndrome or simply short gut) can be caused by the surgical removal of the small intestines. It usually develops in those having had half or more of their small intestines removed.^[127] Diarrhea is the main symptom of short bowel syndrome, however other symptoms may include cramping, bloating, and heartburn. Short bowel syndrome is treated with changes in diet, intravenous feeding, vitamin and mineral supplements, and treatment with medications. Another complication following surgery for Crohn's disease in which the terminal ileum has been removed is the development of excessive watery diarrhea. This is usually thought due to an inability of the ileum to reabsorb bile acids after resection of the terminal ileum and was the first type of bile acid malabsorption recognized.^[128]

In some cases of SBS, intestinal transplant surgery may be considered; though the number of transplant centres offering this procedure is quite small and it comes with a high risk due to the chance of infection and rejection of the transplanted intestine.^[129]

Alternative medicine

More than half of people with Crohn's disease have tried complementary or alternative therapy.^[130] These include diets, probiotics, fish oil and other herbal and nutritional supplements. Some scientists have suggested more research into these is needed to discriminate between effective therapies and "pseudo" therapies that can be ineffective.^[131]

• Acupuncture is used to treat inflammatory bowel disease in China, and is being used more frequently in Western society.^[132] There is insufficient evidence to recommend the use of acupuncture, though further studies are warranted.^[133]
• Homeopathy is frequently used in Germany as a treatment for Crohn's disease, though no clinical trials exist that demonstrate homeopathy is effective.^[134]

Prognosis

Crohn's disease is a chronic condition for which there is no cure. It is characterised by periods of improvement followed by episodes when symptoms flare up. With treatment, most people achieve a healthy weight, and the mortality rate for the disease is relatively low. However, Crohn's disease is associated with an increased risk of small bowel and colorectal carcinoma, including bowel cancer.^[135] It can vary from being benign to very severe and people with CD could experience just one episode or have continuous symptoms. It usually reoccurs, although some people can remain disease free for years or decades. Most live a normal lifespan.^[136]

Complications

Complications

[ v t e ]		Crohn's disease	Ulcerative colitis
Nutrient deficiency		Higher risk
Colon cancer risk		Slight	Considerable
Prevalence of extraintestinal complications[137]
Iritis/uveitis	Females	2.2%	3.2%
	Males	1.3%	0.9%
Primary sclerosing cholangitis	Females	0.3%	1%
	Males	0.4%	3%
Ankylosing spondylitis	Females	0.7%	0.8%
	Males	2.7%	1.5%
Pyoderma gangrenosum	Females	1.2%	0.8%
	Males	1.3%	0.7%
Erythema nodosum	Females	1.9%	2%
	Males	0.6%	0.7%

Crohn's disease can lead to several mechanical complications within the intestines, including obstruction, fistulae, and abscesses. Obstruction typically occurs from strictures or adhesions that narrow the lumen, blocking the passage of the intestinal contents. Fistulae can develop between two loops of bowel, between the bowel and bladder, between the bowel and vagina, and between the bowel and skin. Abscesses are walled off collections of infection, which can occur in the abdomen or in the perianal area. Crohn's is responsible for 10% of vesicoenteric fistulae, and is the most common cause of ileovesical fistulae.^[138]

Crohn's disease also increases the risk of cancer in the area of inflammation. For example, individuals with Crohn's disease involving the small bowel are at higher risk for small intestinal cancer. Similarly, people with Crohn's colitis have a relative risk of 5.6 for developing colon cancer.^[139] Screening for colon cancer with colonoscopy is recommended for anyone who has had Crohn's colitis for at least eight years.^[140] Some studies suggest there is a role for chemoprotection in the prevention of colorectal cancer in Crohn's involving the colon; two agents have been suggested, folate and mesalaminepreparations.^[141]

Individuals with Crohn's disease are at risk of malnutrition for many reasons, including decreased food intake and malabsorption. The risk increases following resection of the small bowel. Such individuals may require oral supplements to increase their caloric intake, or in severe cases, total parenteral nutrition (TPN). Most people with moderate or severe Crohn's disease are referred to a dietitian for assistance in nutrition.^[142]

Crohn's disease can cause significant complications, including bowel obstruction, abscesses, free perforation and hemorrhage.^[143]

Crohn's disease can be problematic during pregnancy, and some medications can cause adverse outcomes for the fetus or mother. Consultation with an obstetrician and gastroenterologist about Crohn's disease and all medications facilitates preventative measures. In some cases, remission occurs during pregnancy. Certain medications can also lower sperm count or otherwise adversely affect a man's fertility.^[144]

Epidemiology

The percentage of people with Crohn's disease has been determined in Norway and the United States and is similar at 6 to 7.1:100,000. The Crohn's and Colitis Foundation of America cites this number as approx 149:100,000; NIH cites 28 to 199 per 100,000.^[145][146] Crohn's disease is more common in northern countries, and with higher rates still in the northern areas of these country.^[147] The incidence of Crohn's disease is thought to be similar in Europe but lower in Asia and Africa.^[145] It also has a higher incidence in Ashkenazi Jews^[1][148] and smokers.^[149]

Crohn's disease has a bimodal distribution in incidence as a function of age: the disease tends to strike people in their teens and 20s, and people in their 50s through to their 70s, and ages in between due to not being diagnosed with Crohn's and being diagnosed instead with irritable bowel syndrome (IBS).^[1][15] It is rarely diagnosed in early childhood. It usually affects females children more severely than males.^[150] However, only slightly more women than men have Crohn's disease.^[151] Parents, siblings or children of people with Crohn's disease are 3 to 20 times more likely to develop the disease.^[152] Twin studies show a concordance of greater than 55% for Crohn's disease.^[153]

History

Inflammatory bowel diseases were described by Giovanni Battista Morgagni (1682–1771) and by Scottish physician T. Kennedy Dalziel in 1913.^[154]

Ileitis terminalis was first described by Polish surgeon Antoni Leśniowski in 1904, however, due to the precedence of Crohn's name in the alphabet, it later became known in the worldwide literature as Crohn's disease.^{[citation needed]} Only in Poland is it still called Leśniowski-Crohn's disease. Burrill Bernard Crohn, an American gastroenterologist at New York City's Mount Sinai Hospital, described fourteen cases in 1932, and submitted them to the American Medical Association under the rubric of "Terminal ileitis: A new clinical entity". Later that year, he, along with colleagues Leon Ginzburg and Gordon Oppenheimer published the case series as "Regional ileitis: a pathologic and clinical entity".^[16]

Research

The Crohn's Allogeneic Transplant Study's investigation team of Seattle is currently undergoing a Phase 2 clinical trial to cure Crohn's disease, involving bone marrow transplant, noting that cases in which bone marrow transplant had been done for a secondary purpose effectively cured the person of Crohn's.^[155]

Researchers at University College London have questioned the wisdom of suppressing the immune system in Crohn's, as the problem may be an underactive rather than an overactive immune system: Their study found that people with Crohn's showed an abnormally low response to an introduced infection, marked by a poor flow of blood to the wound, and the response improved when the they were given sildenafil citrate.^[39]

Recent studies using helminthic therapy or hookworms to treat Crohn's Disease and other (non-viral) auto-immune diseases seem to yield promising results.^[156]

Numerous preclinical studies demonstrate that activation of the CB1 and CB2 cannabinoid receptors exert biological functions on the gastrointestinal tract.^[157] Activation of CB1 and CB2 receptors in animals has shown a strong anti-inflammatory effect.^[158] Cannabinoids and/or modulation of the endocannabinoid system is a novel therapeutic means for the treatment of numerous GI disorders, including inflammatory bowel diseases like Crohn's disease.^[159]

• Methotrexate is a folate anti-metabolite drug that is also used for chemotherapy. It is useful in maintenance of remission for those no longer taking corticosteroids.^[160]
• Metronidazole and ciprofloxacin are antibiotics used to treat Crohn's that have colonic or perianal involvement, although, in the United States, this use has not been approved by the Food and Drug Administration (FDA).^[161] They are also used for treatment of complications, including abscesses and other infections accompanying Crohn's disease.^[15]
• Thalidomide has shown response in reversing endoscopic evidence of disease.^[162]

References

External links

Wikimedia Commons has media related to Crohn's disease.

• Crohn's disease on the Open Directory Project

v t e Inflammatory bowel disease: Crohn's disease and ulcerative colitis Main Biological therapy for inflammatory bowel disease Management of Crohn's disease Crohn's Disease Activity Index Anatomical terms Abdominal pain Anal abscess Erythema nodosum Fistula Granuloma Ileum Ileitis Malabsorption Proctitis Protein losing enteropathy Pyoderma gangrenosum Sacroiliitis Short bowel syndrome Small bowel obstruction Stenosis History Giovanni Battista Morgagni Burrill Bernard Crohn Organizations Crohn's and Colitis Foundation of America National Society for Colitis and Crohn's Disease The Crohn's and Colitis Foundation of Canada People List of people diagnosed with Crohn's disease List of people diagnosed with ulcerative colitis Deaths from Crohn's disease M: DIG anat (t, g, p)/phys/devp/enzy noco/cong/tumr, sysi/epon proc, drug (A2A/2B/3/4/5/6/7/14/16), blte

v t e Digestive system, Digestive disease, Gastroenterology (primarily K20–K93, 530–579) Upper GI tract Esophagus Esophagitis Candidal Herpetiform Rupture Boerhaave syndrome Mallory-Weiss syndrome UES Zenker's diverticulum LES Barrett's esophagus Esophageal motility disorder Nutcracker esophagus Achalasia Diffuse esophageal spasm Gastroesophageal reflux disease (GERD) Laryngopharyngeal reflux (LPR) Esophageal stricture Megaesophagus Stomach Gastritis Atrophic Ménétrier's disease Gastroenteritis Peptic (gastric) ulcer Cushing ulcer Dieulafoy's lesion Dyspepsia Pyloric stenosis Achlorhydria Gastroparesis Gastroptosis Portal hypertensive gastropathy Gastric antral vascular ectasia Gastric dumping syndrome Gastric volvulus Lower GI tract: Intestinal/ Enteropathy Small intestine (Duodenum/Jejunum/Ileum) Enteritis Duodenitis Jejunitis Ileitis Peptic (duodenal) ulcer Curling's ulcer Malabsorption: Coeliac Tropical sprue Blind loop syndrome Small bowel bacterial overgrowth syndrome Whipple's Short bowel syndrome Steatorrhea Milroy disease bile acid malabsorption Large intestine (Appendix/Colon) Appendicitis Colitis Pseudomembranous Ulcerative Ischemic Microscopic Collagenous Lymphocytic Functional colonic disease IBS Intestinal pseudoobstruction / Ogilvie syndrome Megacolon / Toxic megacolon Diverticulitis/Diverticulosis Large and/or small Enterocolitis Necrotizing IBD Crohn's disease Vascular: Abdominal angina Mesenteric ischemia Angiodysplasia Bowel obstruction: Ileus Intussusception Volvulus Fecal impaction Constipation Diarrhea Infectious Intestinal adhesions Rectum Proctitis Radiation proctitis Proctalgia fugax Rectal prolapse Anismus Anal canal Anal fissure/Anal fistula Anal abscess Anal dysplasia Pruritus ani GI bleeding/BIS Upper Hematemesis Melena Lower Hematochezia Accessory Liver Hepatitis Viral hepatitis Autoimmune hepatitis Alcoholic hepatitis Cirrhosis PBC Fatty liver NASH Vascular Budd-Chiari syndrome Hepatic veno-occlusive disease Portal hypertension Nutmeg liver Alcoholic liver disease Liver failure Hepatic encephalopathy Acute liver failure Liver abscess Pyogenic Amoebic Hepatorenal syndrome Peliosis hepatis Metabolic Disorders Wilson's Disease Hemochromatosis Gallbladder Cholecystitis Gallstones/Cholecystolithiasis Cholesterolosis Rokitansky-Aschoff sinuses Postcholecystectomy syndrome Porcelain gallbladder Bile duct/ Other biliary tree Cholangitis PSC Secondary sclerosing cholangitis Ascending Cholestasis/Mirizzi's syndrome Biliary fistula Haemobilia Gallstones/Cholelithiasis Common bile duct Choledocholithiasis Biliary dyskinesia Sphincter of Oddi dysfunction Pancreatic Pancreatitis Acute Chronic Hereditary Pancreatic abscess Pancreatic pseudocyst Exocrine pancreatic insufficiency Pancreatic fistula Abdominopelvic Hernia Diaphragmatic Congenital Hiatus Inguinal Indirect Direct Umbilical Femoral Obturator Spigelian Lumbar Petit's Grynfeltt-Lesshaft Undefined location Incisional Internal hernia Peritoneal Peritonitis Spontaneous bacterial peritonitis Hemoperitoneum Pneumoperitoneum M: DIG anat (t, g, p)/phys/devp/enzy noco/cong/tumr, sysi/epon proc, drug (A2A/2B/3/4/5/6/7/14/16), blte

v t e Oral and maxillofacial pathology (K06, K11–K14, 523, 527–529) Lips Cheilitis Angular Actinic Plasma cell Herpes labialis Trumpeter's wart Tongue Glossitis Geographic tongue Median rhomboid glossitis Transient lingual papillitis Fissured tongue Black hairy tongue Caviar tongue Macroglossia Hypoglossia Ankyloglossia Crenated tongue Oral mucosa Oral ulceration Stomatitis Aphthous Herpetic Nicotinic Denture-related Erythroplakia Leukoplakia Hairy leukoplakia Leukoedema White sponge nevus Burning mouth syndrome Fordyce spots Lichen planus Morsicatio buccarum Linea alba Behçet syndrome Angina bullosa haemorrhagica Melanocytic oral lesion Oral melanosis Recurrent intraoral herpes simplex infection Plasmoacanthoma Oral florid papillomatosis Oral candidiasis Herpangina Focal epithelial hyperplasia Epulis fissuratum Teeth (pulp, dentin, enamel) Dental caries Dentin hypersensitivity Pulpitis Pulp necrosis Pulp polyp Pulp calcification Fluorosis Hypodontia Hyperdontia Macrodontia Microdontia Dilaceration Taurodontism Fusion Gemination Concrescence Amelogenesis imperfecta Dentinogenesis imperfecta Dentin dysplasia Regional odontodysplasia Tooth wear Attrition Erosion Abrasion Abfraction Resorption Premature eruption Delayed eruption Impaction Odontome Dens in dente Odontogenic tumors Keratocystic odontogenic tumour Cracked tooth syndrome Periodontium (gingiva, Periodontal ligament, cementum, alveolus) Gingivitis Desquamative gingivitis Plasma cell gingivitis Epulis Pyogenic granuloma Gingival enlargement Periodontitis Pericoronitis Necrotizing periodontal diseases Acute necrotizing ulcerative gingivitis Periodontal abscess Hypercementosis Hypocementosis Periapaical, mandibular and maxillary hard tissues Periapical periodontitis Periapical abscess Alveolar osteitis Torus palatinus Torus mandibularis Cherubism Paget's disease of bone Mandibular fracture Stafne defect Osteomyelitis Osteonecrosis Bisphosphonate-associated Neuralgia-inducing cavitational osteonecrosis Osteoradionecrosis Temporomandibular joints and muscles of mastication Temporomandibular joint dysfunction Bruxism Mandibular dislocation Salivary glands Sialadenitis Parotitis Chronic sclerosing sialadenitis Sialolithiasis Mucocele Ranula Sjögren's syndrome Sialocele Benign lymphoepithelial lesion Necrotizing sialometaplasia Salivary gland neoplasm Pleomorphic adenoma Orofacial soft tissues Ludwig's angina Cutaneous sinus of dental origin Cystic hygroma Velopharyngeal inadequacy Actinomycosis Orofacial granulomatosis Melkersson–Rosenthal syndrome Pyostomatitis vegetans Oral Crohn's disease Perioral dermatitis Noma M: MOU anat/devp noco/cofa (c)/cogi/tumr, sysi proc (peri), drug (A1)