Primary sclerosing cholangitis

Primary sclerosing cholangitis

Cholangiogram of primary sclerosing cholangitis.
Classification and external resources
Specialty Gastroenterology
ICD-10 K83.0
ICD-9-CM 576.1
OMIM 613806
DiseasesDB 10643
MedlinePlus 000285
eMedicine med/3556
Patient UK Primary sclerosing cholangitis
MeSH D015209

Primary sclerosing cholangitis (PSC) is a disease of the bile ducts that causes inflammation and obliterative fibrosis of bile ducts inside and/or outside of the liver. This pathological process impedes the flow of bile to the intestines and can ultimately lead to cirrhosis of the liver, liver failure, and other complications, including but not limited to bile duct and liver cancer. The underlying cause of the inflammation remains unknown, but elements of autoimmunity and microbial dysbiosis have been described[1] and are suggested by the fact that approximately 75% of those with PSC also have inflammatory bowel disease (IBD), most often ulcerative colitis.[2] The most definitive treatment for PSC is liver transplantation.

Signs and symptoms

A video explanation of primary sclerosing cholangitis

Many patients with PSC are asymptomatic, but a substantial proportion will have debilitating signs and symptoms of the disease.[3] These may include:

Cause

Primary sclerosing cholangitis is idiopathic (having no known cause). While thought to be an autoimmune disease, it does not demonstrate a clear response to immunosuppressants. Thus, many experts believe it to be a complex, multifactorial (including immune-mediated) disorder, and perhaps one that encompasses several different hepatobiliary diseases.[6][7]

Recent data have provided novel insights suggesting: 1) an important association between the intestinal microbiota and PSC[8][9][10][11] and 2) a process referred to as cellular senescence and the senescence-associated secretory phenotype (SASP) in the pathogenesis of PSC.[12][13] In addition, there are longstanding, well-recognized associations between PSC and Human leukocyte antigen [HLA] alleles (e.g. A1, B8, and DR3).[1]

Pathophysiology

PSC is believed to develop due to inflammation of the bile ducts (cholangitis), with consequent stricturing (i.e. narrowing) and hardening (sclerosis) of these ducts due to scar formation, be it inside and/or outside of the liver.[14] The resulting scarring of the bile ducts obstructs the flow of bile, which further perpetuates bile duct and liver injury. Chronic impairment of bile flow due to blockage and dysfunctional bile transport (cholestasis) causes progressive biliary fibrosis and ultimately biliary cirrhosis and liver failure.[15]

The physiological function of bile is to assist in the breakdown and absorption of fat in the intestinal tract; a relative deficiency of bile can lead to fat malabsorption and deficiencies of fat-soluble vitamins (A, D, E, K).

Diagnosis

PSC is generally diagnosed on the basis of having at least two of three clinical: serum alkaline phosphatase (ALP) > 1.5x the upper limit of normal, cholangiography demonstrating biliary strictures or irregularity consistent with PSC, and liver histology (if available). Historically, a cholangiogram would be obtained via endoscopic retrograde cholangiopancreatography (ERCP), which typically reveals "beading" (alternating strictures and dilation) of the bile ducts inside and/or outside the liver. Currently, the preferred option for diagnostic cholangiography, given its non-invasive yet highly accurate nature, is magnetic resonance cholangiopancreatography (MRCP), a magnetic resonance imaging technique. MRCP has unique strengths, including high spatial resolution, and can even be used to visualize the biliary tract of small animal models of PSC.[16]

Most people with PSC have evidence of autoantibodies and abnormal immunoglobulin levels.[17] For example, approximately 80% of people with PSC have perinuclear anti-neutrophil cytoplasmic antibodies; however, this and other immunoglobulin findings are not specific to those with PSC and are of unclear clinical significance/consequence. Antinuclear antibodies and anti-smooth muscle antibody are found in 20%-50% of PSC patients and, likewise, are not specific for the disease but may identify a subgroup of PSC patients who also have auotimmune hepatitis (i.e. PSC-AIH overlap syndrome).[1]

Other markers which may be measured and monitored are a complete blood count, serum liver enzymes, bilirubin levels (usually grossly elevated), kidney function, and electrolytes. Fecal fat measurement is occasionally ordered when symptoms of malabsorption (e.g. gross steatorrhea) are prominent.

The differential diagnosis can include primary biliary cholangitis (formerly referred to as primary biliary cirrhosis), drug induced cholestasis, cholangiocarcinoma, IgG4-associated disease, post-liver transplantation non-anastomotic biliary strictures,[18] and HIV-associated cholangiopathy.[19]

Management

There is no FDA-approved pharmacologic treatment for PSC. Some experts recommend a trial of ursodeoxycholic acid (UDCA), a bile acid occurring naturally in small quantities in humans, as it has been shown to lower elevated liver enzyme numbers in patients with PSC and has proven effective in other cholestatic liver diseases. However, UDCA has yet to be shown to clearly lead to improved liver histology and adverse event-free survival.[3][20]

Treatment for patients with PSC also includes therapies to relieve itching (antipruritics) (e.g. the bile acid sequestrant (cholestyramine), antibiotics to treat episodes of acute cholangitis, and vitamin supplements, as people with PSC are often deficient in fat-soluble vitamins (vitamin A, vitamin D, vitamin E, and vitamin K).

In some cases, ERCP with balloon dilation, with or without stenting, may be necessary in order to open major blockages (dominant strictures) in the biliary tree. ERCP and specialized techniques may also be needed to help distinguish between a benign PSC stricture a bile duct cancer (cholangiocarcinoma)[21]

Liver transplantation is the only proven long-term treatment of PSC. Indications for transplantation include recurrent bacterial cholangitis, decompensated cirrhosis, hepatocellular carcinoma, hilar cholangiocarcinoma, and complications of portal hypertension. Unfortunately, not all patients are candidates for liver transplantation, and some will experience disease recurrence afterward.[6]

Despite there being no curative treatment at present, it is important to note that there are several clinical trials underway that aim to slow progression of this liver disease.[22]

Prognosis

PSC carries an estimated median liver transplant-free survival time (from diagnosis) of approximately 15 years.[23][24] Various models have been developed to help predict survival, but their use is generally best suited for research and not clinical purposes. Recently, normalization of serum alkaline phosphatase has been shown to be an accurate and non-invasive predictor of favorable long-term outcomes.[25]

Related diseases

Primary sclerosing cholangitis is associated with cholangiocarcinoma,[26] a cancer of the biliary tree, for which the lifetime risk among patients with PSC is 10-15%.[27] This represents a 160-fold greater risk of developing cholangiocarcinoma compared to the general population.[27] Surveillance for cholangiocarcinoma in patients with PSC is encouraged, with some experts recommending annual surveillance,[28] but there is no official consensus on the modality and interval of choice. Colon cancer is also associated with PSC.[26]

PSC has a significant association with ulcerative colitis, an inflammatory bowel disease primarily affecting the large intestine. As many as 5% of patients with inflammatory bowel disease (IBD), especially ulcerative colitis (UC), may be co-diagnosed with PSC[29] and approximately 70% of people with primary sclerosing cholangitis have ulcerative colitis.[15] Those with PSC and IBD are at approximately 30-fold increased risk of developing colorectal cancer; therefore, regular surveillance is recommended.[30] The presence of colitis is associated with a greater risk of liver disease progression and bile duct cancer (cholangiocarcinoma).[31] Close monitoring of PSC patients is vital.

Other diseases with which PSC is associated include osteoporosis (hepatic osteodystrophy) and hypothyroidism.

Epidemiology

There is a 2-3:1 male-to-female predilection in primary sclerosing cholangitis.[15] PSC can affect men and women at any age, although it is commonly diagnosed in the fourth decade of life, most often in the presence of inflammatory bowel disease (IBD).[14] PSC progresses slowly and is often asymptomatic, so it can be present for years before it is diagnosed and before it causes clinically significant consequences. There is relatively little data on the prevalence and incidence of primary sclerosing cholangitis, with studies in different countries showing annual incidence of 0.068–1.3 per 100,000 people and prevalence 0.22–8.5 per 100,000; given that PSC is closely linked with ulcerative colitis, it is likely that the risk is higher in populations where UC is more common.[32] In the United States, an estimated 25,000 individuals have PSC.

See also

References

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  2. Sleisenger, MH (2006). Sleisenger and Fordtran's gastrointestinal and liver disease: pathophysiology, diagnosis, management (8th ed.). Philadelphia: Saunders.
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  4. Tabibian JH, Yang JD, Baron TH, Kane SV, Enders FB, Gostout CJ. Weekend Admission for Acute Cholangitis Does Not Adversely Impact Clinical or Endoscopic Outcomes. Dig Dis Sci. 2016 Jan;61(1):53-61. doi: 10.1007/s10620-015-3853-z. Epub 2015 Sep 21.
  5. Tabibian JH, Abu Dayyeh BK, Gores GJ, Levy MJ (2015). "A novel, minimally-invasive technique for management of peristomal varices". Hepatology. doi:10.1002/hep.27925.
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External links

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