Autoimmune Hepatitis Cleveland Clinic
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Andre Fialho, MD
William D. Carey, MD Autoimmune hepatitis (AIH) is a chronic inflammatory condition of the liver of unknown etiology identified in the 1940s and formerly called chronic active hepatitis. Autoimmune hepatitis is characterized by liver transaminase elevation in the presence of autoantibodies, elevated gamma globulin levels, interface hepatitis on histology, and a great response to corticosteroids. Next: Epidemiology Epidemiology
Minocycline
Halothane Probable Atorvastatin
Isoniazide
Diclofenac
Propylthiouracil
Infliximab Uncertain Adalimumab
Cephalexin
Fenofibrate
Indomethacin
Imatinib
Rosuvastatin
Meloxicam
Methylphenidate
There is a strong association of AIH with other autoimmune diseases and up to 26% to 49% of the individuals with AIH will have concomitant autoimmune diseases. Autoimmune hepatitis type 1 is associated with autoimmune thyroiditis, Grave's disease, and ulcerative colitis while AIH type 2 is associated with diabetes mellitus type 1, vitiligo, and autoimmune thyroiditis.
In the majority of cases, AIH diagnosis can be made by using Table 2. When patients do not meet all the criteria in Table 2 or have atypical features, the diagnosis of AIH becomes less certain and they should be referred to a gastroenterologist or hepatologist. Table 2: Diagnosis of Autoimmune Hepatitis Diagnostic Criteria Elevation of AST/ALT 5–10 times upper limit of normal Gamma globulins or IgG levels ≥1.5 times upper limit of normal Positive ANA, ASMA or Anti-LKM1 in titers >1:80 Female sex Negative markers for hepatitis A,B and C and Wilson's disease Alcohol consumption of less than 25 g/day Absence of hepatotoxic drugs Interpretation of Table 2: Autoimmune hepatitis is diagnosed when all of the above diagnostic criteria are met. Liver biopsy under these circumstances can be relevant for assessing severity of AIH. If some of the criteria above are not met, diagnosis of AIH is less certain and patients should be referred to a gastroenterologist or hepatologist before starting treatment. ANA = antinuclear antibody; ALT = alanine aminotransferase; ASMA = antismooth-muscle antibody; AST = aspartate aminotransferase; IgG = immunoglobulin G; anti-LKM1 = anti-liver kidney microsomal antibody type 1.
*Onset in adults, frequently acute (6% fulminant), corticosteroid responsive, cirrhosis in 35%
**Onset in childhood (age 2 to 14 years), usually indolent, more often corticosteroid refractory; cirrhosis in 80% AIH = autoimmune hepatitis; ANA = antinuclear antibody; Anti-LC1 = anti-liver cytosol type 1 antibody; anti-LKM1 = anti-liver-kidney microsomal antibody type 1; anti-LKM3 = anti-liver-kidney microsomal antibody type 3; pANCA = perinuclear anti-neutrophil cytoplasmic antibody; anti-SLA/LP = anti-soluble liver antigen/liver pancreas antibody; ASMA = antismooth-muscle antibody. Approximately 20% of patients may lack ANA, ASMA, and anti-LKM1. In these cases, additional antibodies may be present such anti soluble liver antibody (anti-SLA), anti-LC1, and anti-liver-kidney microsomal antibody type 3 (anti-LKM3). The presence of anti-SLA can occur in AIH type 1 and type 2 and is associated with severe disease and worse prognosis. Both LC1 and LKM3 occur in type 2 AIH. These antibodies are not readily available in many institutions, hence the diagnosis of AIH when typical antibodies are negative will most often rely on histologic features. Atypical perinuclear-anti-neutrophil cytoplasmic antibodies (p-ANCA) can also be positive in AIH type 1 and may be an additional clue for the diagnosis when the conventional antibodies are negative. Antimitochondrial antibody (AMA) in low titers can occur in AIH and this does not imply superimposed PBC.
Liver toxicity
Myelosuppression
Pancreatitis
Malignancy (most often lymphoma)
Rash Pregnancy
Malignancy
Leukopenia <2.5 x 109/L
Thrombocytopenia <50 x 109
Known complete TPMT deficiency Budesonide Usually none
Cosmetic changes (moon faces, acne and hirsutism) Cirrhosis Prednisone Osteoporosis
Emotional instability
Diabetes
Hypertension
Cosmetic changes (see budesonide)
Cataracts
Weight gain Vertebral compression
Psychosis
Brittle diabetes
Uncontrolled hypertension TPMT = thiopurine methyltransferase. The treatment of AIH consists of 2 phases: 1) induction of remission and 2) maintenance of remission. Please refer to Table 5 for detailed treatment regimens in each phase. Table 5: Most Common Treatment Options for Autoimmune Hepatitis
Combination Treatment
Prednisone + Azathioprine Combination Treatment
Budesonide + Azathioprine Prednisone Monotherapy Induction Week 1 30 mg/d + 50 mg/d 9 mg/d + 50 mg/d Prednisone 60 mg/d Week 2 25 mg/d + 50 mg/d 9 mg/d + 50 mg/d Prednisone 40 mg/d Week 3 20 mg/d + 50 mg/d 6 mg/d + 50 mg/d Prednisone 30 mg/d Week 4 15 mg/d + 50 mg/d 6 mg/d + 50 mg/d Prednisone 20 mg/d Maintenance First 12 months Prednisone 10 mg/d + Azathioprine 50 mg/d Budesonide 6 mg/d + Azathioprine 50 mg/d Prednisone 20 mg/d or less for at least 24 months 12-24 months Prednisone taper 2.5 mg/week until withdrawal. Thereafter azathioprine monotherapy 50-100 mg/day Consider budesonide taper until withdrawal. Thereafter azathioprine monotherapy 50-100 mg/day
Treatment Withdrawal
After 24 months of complete remission
OR
Liver biopsy showing absence of inflammation Same Same Indication
Preferred over prednisone monotherapy as fewer side effects Potential frontline therapy
Patients with obesity, acne, diabetes, and hypertension may benefit Reserved for patients who cannot take azathioprine Disadvantages
Side effects of prednisone, although less often and less severe than high-dose prednisone Expensive
Fewer studies showing efficacy Severe corticosteroid induced side effects Induction Phase In the induction phase, prednisone 30 mg per day plus azathioprine 50 mg per day is started for 1 week. This is followed by a prednisone taper over the course of 4 weeks with a fixed azathioprine dose of 50 mg per day to achieve a dose of prednisone 10 mg per day plus azathioprine 50 mg per day as shown in Table 5. Should budesonide plus azathioprine be selected, induction is achieved with combination of budesonide 3 mg three times daily plus azathioprine 50 mg per day for 2 weeks, followed by a budesonide 3 mg twice daily thereafter. Maintenance Phase For those receiving prednisone plus azathioprine, maintenance phase begins typically after 4 weeks, when the dose of prednisone 10 mg per day plus azathioprine 50 mg per day is started. This dose is continued for at least 1 full year. The daily maintenance dose of prednisone should remained fixed, as dose titration according to liver transaminases or alternate day schedules of prednisone are associated with incomplete histological improvement despite laboratory improvement. After 1 year of controlled disease, consideration can be given to withdrawal of prednisone while continuing azathioprine. Thereafter azathioprine monotherapy is continued for long-term maintenance. Patients can often be maintained on doses of azathioprine monotherapy of 50 mg per day to 100 mg per day with normal liver enzymes. Azathioprine doses of less than 100 mg per day have the advantage of less toxicity, particularly less leukopenia. Table 5 shows the medical regimen for AIH. If budesonide is used, the maintenance dose is 6 mg twice daily in combination with azathioprine 50 mg per day. One may consider tapering budesonide while maintaining azathioprine 50 mg per day to 100 mg per day (azathioprine monotherapy) after 12 months, but there are currently no studies on the long term effect of azathioprine monotherapy after budesonide plus azathioprine combination.
Visitation, mask requirements and COVID-19 information Digestive Disease & Surgery Institute
Autoimmune Hepatitis
Appointments 216.444.7000 Our Doctors Contact Us Print Full Guide DefinitionDefinition
Andrea Fialho, MDAndre Fialho, MD
William D. Carey, MD Autoimmune hepatitis (AIH) is a chronic inflammatory condition of the liver of unknown etiology identified in the 1940s and formerly called chronic active hepatitis. Autoimmune hepatitis is characterized by liver transaminase elevation in the presence of autoantibodies, elevated gamma globulin levels, interface hepatitis on histology, and a great response to corticosteroids. Next: Epidemiology Epidemiology
Epidemiology
Autoimmune hepatitis occurs worldwide but the exact incidence and prevalence of the disease in the United States is unknown. The point prevalence and incidence of AIH in Northern Europeans is approximately 18 per 100,000 people per year and 1.1 per 100,000 people per year, respectively, and it is assumed that this data can be extrapolated to the North American population. Interestingly the prevalence of AIH in Native Alaskan population is much higher, with a point prevalence of 42 per 100,000 people/year. Autoimmune hepatitis has a female predominance and a bimodal age distribution with 2 peaks, 1 in childhood and another in the 5th decade. However AIH occurs in both genders and in all age groups and there have been reports of newly diagnosed AIH in patients 80 years of age.Subtypes
Autoimmune hepatitis is subdivided in 2 types, according to the pattern of autoantibodies. Although management does not differ between these 2 types, there is a prognostic value. Type 1 AIH: This is the most common type in the United States, accounting for 96% of the AIH cases in North America, has a female to male ratio of 4 to 1 and a great response to corticosteroids. It is characterized by the presence of antinuclear antibody (ANA) and antismooth-muscle antibody (ASMA). Type 2 AIH: This type occurs most often in Europe and the patients tend to be younger (usually less than 14 years old), have more severe disease, worse response to corticosteroids, and relapse more often. Type 2 AIH accounts for only 4% of the AIH cases in North America. It is characterized by the presence of anti-liver kidney microsomal antibody type 1 (anti-LKM1) and/or anti-liver cytosol type 1 (anti-LC1) autoantibodies.Genetics and Predisposing Factors
Autoimmune hepatitis is thought to result from an environmental trigger in a genetically predisposed individual, leading to loss of tolerance of T lymphocytes with subsequent hepatocyte attack. It is a polygenic disease and does not follow a Mendelian distribution. Therefore there is no need to screen family members of patients with AIH. There is a strong genetic association with the alleles of the major histocompatibility complex class II. The presence of human leukocyte antigen (HLA) genes HLA DRB1*03 and HLA DRB1*04 predisposes to AIH type 1 and affect the disease course and response to treatment. Individuals who are positive for HLA DRB1*03 are younger, respond less favorably to corticosteroid therapy, and progress more often to liver failure. On the other hand, the presence of HLA DRB1*04 is associated with higher rates of concomitant autoimmune disorders. Autoimmune hepatitis can also be associated with autoimmune polyendocrinopathy candidiasis ectodermal dystrophy syndrome, an autosomal recessive disease characterized by hypoparathyroidism, adrenal insufficiency, and chronic mucocutaneous candidiasis. Autoimmune polyendocrinopathy candidiasis ectodermal dystrophy is the only AIH-associated disease that follows a Mendelian pattern of inheritance and genetic counseling should be offered for patients and family members. Viruses such as hepatitis A and Epstein Barr virus have been proposed as a potential environmental triggers for AIH through molecular mimicry. However available data consists mainly of case reports. Drugs such as propylthiouracil, minocycline, and nitrofurantoin can cause drug-induced autoimmune-like hepatitis (DIAH) which is clinically, biochemically, and histologically indistinguishable from AIH but is a different entity. As in AIH, DIAH is characterized by female predominance, elevated liver transaminases (aspartate aminotransferase [AST], alanine aminotransferase [ALT]) with minimal alkaline phosphatase elevation, positive autoantibodies, and interface hepatitis on liver biopsy. Similarly to AIH, ANA is positive in 70% to 80% of the cases and ASMA is positive in 40% to 50% of the cases. In addition to drug discontinuation, DIAH is treated with steroids and response is excellent. In contrast to AIH, 100% of the patients with DIAH will be able to have steroids withdrawn without relapse.Table 1 shows the most common drugs associated with DIAH. Table 1: Drugs Associated With Drug-Induced Autoimmune-Like Hepatitis Association Drug Strong NitrofurantoinMinocycline
Halothane Probable Atorvastatin
Isoniazide
Diclofenac
Propylthiouracil
Infliximab Uncertain Adalimumab
Cephalexin
Fenofibrate
Indomethacin
Imatinib
Rosuvastatin
Meloxicam
Methylphenidate
There is a strong association of AIH with other autoimmune diseases and up to 26% to 49% of the individuals with AIH will have concomitant autoimmune diseases. Autoimmune hepatitis type 1 is associated with autoimmune thyroiditis, Grave's disease, and ulcerative colitis while AIH type 2 is associated with diabetes mellitus type 1, vitiligo, and autoimmune thyroiditis.
Natural History
Autoimmune hepatitis was once a lethal condition with a dismal prognosis. Treatment with corticosteroids has changed the course of the disease and nowadays AIH can be considered a disease with relatively good prognosis in responsive patients. Most of the data on untreated AIH comes from studies pursued in the 1970s, when the benefit of corticosteroids was established. Without treatment, approximately 40% to 50% of the individuals with severe disease will die within 6 months to 5 years. Treatment with steroids has dramatically changed the course of the disease. Most patients respond to therapy and the 10-year survival rate is approximately 83.8% to 94%. Thus prompt recognition of the disease and initiation of treatment is critical. Previous: Definition Next: Symptoms SymptomsSymptoms
The clinical presentation of autoimmune hepatitis varies from asymptomatic to acute liver failure. Symptoms of anorexia, arthralgias, maculopapular rash, and fatigue are typical but not always present. Most patients will have an insidious onset with constitutional symptoms, 25% of patients will be asymptomatic and diagnosed incidentally, and 30% of patients will have acute hepatitis manifestations, the later occurring more often in younger patients. Severe acute hepatitis similar to viral hepatitis can occur. Fulminant hepatic failure is rare and appears to be more common in AIH type 2. Previous: Epidemiology Next: Diagnosis DiagnosisDiagnosis
No single test is diagnostic for AIH. The diagnosis of AIH is based on a combination of characteristic clinical features and typical laboratory abnormalities. Other causes of chronic hepatitis should be excluded, including alcohol induced hepatitis, drug-induced hepatitis, and viral hepatitis. Table 2 shows simplified diagnostic criteria for AIH and Figure 1 shows a simplified diagnostic algorithm for AIH. Figure 1: Simplified diagnostic algorithm for autoimmune hepatitis. AIH = autoimmune hepatitis; ANA = antinuclear antibody; ASMA = antismooth-muscle antibody; IgG = immunoglobulin G; anti-LC1 = anti-liver cytosol type 1 antibody; anti-LKM1 = anti-liver-kidney microsomal antibody type 1; anti-LKM3 = anti-liver-kidney microsomal antibody type 3; NASH = nonalcoholic steatohepatitis; PBC = primary biliary cirrhosis; PSC = primary sclerosing cholangitis; anti-SLA/LP = anti-soluble liver antigen/liver-pancreas antibody.In the majority of cases, AIH diagnosis can be made by using Table 2. When patients do not meet all the criteria in Table 2 or have atypical features, the diagnosis of AIH becomes less certain and they should be referred to a gastroenterologist or hepatologist. Table 2: Diagnosis of Autoimmune Hepatitis Diagnostic Criteria Elevation of AST/ALT 5–10 times upper limit of normal Gamma globulins or IgG levels ≥1.5 times upper limit of normal Positive ANA, ASMA or Anti-LKM1 in titers >1:80 Female sex Negative markers for hepatitis A,B and C and Wilson's disease Alcohol consumption of less than 25 g/day Absence of hepatotoxic drugs Interpretation of Table 2: Autoimmune hepatitis is diagnosed when all of the above diagnostic criteria are met. Liver biopsy under these circumstances can be relevant for assessing severity of AIH. If some of the criteria above are not met, diagnosis of AIH is less certain and patients should be referred to a gastroenterologist or hepatologist before starting treatment. ANA = antinuclear antibody; ALT = alanine aminotransferase; ASMA = antismooth-muscle antibody; AST = aspartate aminotransferase; IgG = immunoglobulin G; anti-LKM1 = anti-liver kidney microsomal antibody type 1.
Laboratory Abnormalities
The major laboratory abnormalities encountered in AIH are elevation of liver transaminases and gamma globulins and the presence of autoantibodies. Liver Enzyme Abnormalities Elevation of liver transaminases less than 500 UI/L with normal alkaline phosphatase is typical. Liver transaminase elevation to 1,000 UI/L resembling acute viral hepatitis and liver ischemia is less common but can occur. An elevation of alkaline phosphatase that is disproportional to transaminase ALT or AST elevation with an alkaline phosphatase to ALT or AST ratio of ≥3 is unusual and should prompt investigation of other causes of liver disease such as drug induced disease, primary biliary cirrhosis (PBC) and primary sclerosing cholangitis (PSC). Individuals with AIH may concomitantly have features of other autoimmune liver diseases such as PSC or PBC, termed overlap syndrome. The overlap syndrome of AIH with PBC or AIH with PSC will be discussed separately further in this chapter. Gamma Globulin Elevation Gamma globulin elevation occurs in 80% of the cases. There is a polyclonal elevation in immunoglobulin (Ig), with a predominant IgG elevation. Along with liver transaminases, gamma globulin levels are important markers of disease activity. Autoantibodies As discussed previously in the epidemiology topic of this chapter, the presence of autoantibodies is common in AIH, most frequently ANA, ASMA, and anti-LKM1. See Table 3 for the differences between AIH type 1 and type 2 with regards to autoantibody profile. It is extremely rare to have the occurrence of antibodies to AIH type 1 (ANA and ASMA) and antibodies to AIH type 2 (anti-LKM1) in the same patient. In the few cases where this situation occurs, the course of disease is similar to AIH type 2. Table 3: Autoantibody Interpretation in Autoimmune Hepatitis AIH type Conventional Autoantibodies Nonconventional Autoantibodies AIH type 1* ANA, ASMA pANCA, anti-SLA/LP AIH type 2** Anti-LKM1 Anti-LC1, anti-LKM3, anti-SLA/LP*Onset in adults, frequently acute (6% fulminant), corticosteroid responsive, cirrhosis in 35%
**Onset in childhood (age 2 to 14 years), usually indolent, more often corticosteroid refractory; cirrhosis in 80% AIH = autoimmune hepatitis; ANA = antinuclear antibody; Anti-LC1 = anti-liver cytosol type 1 antibody; anti-LKM1 = anti-liver-kidney microsomal antibody type 1; anti-LKM3 = anti-liver-kidney microsomal antibody type 3; pANCA = perinuclear anti-neutrophil cytoplasmic antibody; anti-SLA/LP = anti-soluble liver antigen/liver pancreas antibody; ASMA = antismooth-muscle antibody. Approximately 20% of patients may lack ANA, ASMA, and anti-LKM1. In these cases, additional antibodies may be present such anti soluble liver antibody (anti-SLA), anti-LC1, and anti-liver-kidney microsomal antibody type 3 (anti-LKM3). The presence of anti-SLA can occur in AIH type 1 and type 2 and is associated with severe disease and worse prognosis. Both LC1 and LKM3 occur in type 2 AIH. These antibodies are not readily available in many institutions, hence the diagnosis of AIH when typical antibodies are negative will most often rely on histologic features. Atypical perinuclear-anti-neutrophil cytoplasmic antibodies (p-ANCA) can also be positive in AIH type 1 and may be an additional clue for the diagnosis when the conventional antibodies are negative. Antimitochondrial antibody (AMA) in low titers can occur in AIH and this does not imply superimposed PBC.
Liver Biopsy
Liver biopsy should be considered for the diagnosis of AIH and it can provide valuable information regarding severity of the disease. The American Association for Study of Liver Diseases recommends a liver biopsy for diagnostic purposes. The hallmark of AIH on histology is interface hepatitis characterized by lymphocytic infiltrate in the portal triad that goes beyond the limiting plate and reaches the bordering hepatocytes. The bile ducts are intact. Interface hepatitis, although commonly seen in AIH, is not pathognomonic and can occur in other liver diseases. Figure 2 outlines the major histologic features of AIH. In severe acute autoimmune hepatitis one should not wait for biopsy results to start treatment, as delay in therapy has been associated with adverse outcomes. Figure 2: Histologic hallmarks of autoimmune hepatitis. (A) Depiction of a normal hepatic lobule, note the clear delineation between the connective tissue of the portal triad and the hepatocytes. In autoimmune hepatitis, (B and C) lymphocytic infiltrate accumulates in the portal triad. Interface hepatitis (C) occurs when the lymphocytes in the portal triad invade the limiting plate spilling around the hepatocytesImaging
There is no role for routine imaging in the diagnosis of AIH. Because patients with inflammatory bowel disease (IBD) and AIH have high rates of PSC, they should have a cholangiographic study once AIH is diagnosed to rule out PSC. Unless otherwise contraindicated, magnetic resonance cholangiopancreatography (MRCP) is usually the test of choice. Previous: Symptoms Next: Treatment TreatmentTreatment
Treatment is directed against inflammation and the cornerstone of therapy is corticosteroid therapy. Treatment is the same for type1 and type 2 AIH. Response to corticosteroid is usually excellent in AIH type 1, with 80% of the patients having normalization of liver function tests.When to Start Treatment
Treatment should be started in patients with significant disease, characterized by at least one of the following: AST or ALT >10 times the upper limit of normal; AST or ALT >5 times the upper limit of normal and IgG >2 times the upper limit of normal; bridging necrosis or multiacinar necrosis on histology. Although uncommon, the presence of incapacitating symptoms (fatigue, arthralgia) has also been proposed as an indication of treatment regardless of laboratory values. In asymptomatic patients with AST, ALT, and gamma globulins/IgG elevations that do not meet the criteria above, the benefit of treatment is less clear. The course of the disease in such patients has not been well established and there is little data to support treatment. Thus in asymptomatic patients with only mild laboratory and histological changes, the decision to start treatment should be individualized and the risks of therapy taken into account. Often treatment in this situation can be postponed and liver tests followed closely. Such patients should always be referred to a hepatologist or gastroenterologist for decision regarding therapy. Asymptomatic patients with inactive disease (minimal or absent inflammation) on liver biopsy or burned out cirrhosis do not benefit from treatment.Treatment Options
The most commonly used initial treatment options are immunosuppressive therapy with either 1) a combination of prednisone and azathioprine, 2) a combination of budesonide and azathioprine or 3) high-dose prednisone monotherapy. The 2 most studied treatment regimens are high dose prednisone monotherapy or combination therapy of prednisone plus azathioprine. Both are equivalent in efficacy of induction of remission, but prednisone monotherapy is associated with higher rates of corticosteroid induced side effects. Hence combination therapy of prednisone and azathioprine should always be preferred unless contraindications to azathioprine exist. More recently, combination therapy of budesonide plus azathioprine is emerging as a potential frontline treatment option for AIH. Budesonide is a corticosteroid that has 90% first-pass metabolism in the liver and thus has fewer systemic side effects than prednisone. This regimen has been compared with combination therapy of azathioprine 50 mg per day plus prednisone in a randomized, controlled trial and was shown to have better clinical and laboratory remission rates with fewer steroid induced side effects at 6 months after initiation of therapy. The main disadvantage of budesonide plus azathioprine combination therapy is that it is more expensive and to date there are no studies evaluating long-term remission with this regimen. It is a valuable option in patients with obesity, acne, diabetes, hypertension, and osteopenia who are at high risk of developing side effects from prednisone. Table 4 shows the main side effects and contraindications of each drug. Table 4: Side Effects and Contraindications of the Most Commonly Used Drugs in Autoimmune Hepatitis Drug Major Side Effects Contraindications Azathioprine Nausea and vomitingLiver toxicity
Myelosuppression
Pancreatitis
Malignancy (most often lymphoma)
Rash Pregnancy
Malignancy
Leukopenia <2.5 x 109/L
Thrombocytopenia <50 x 109
Known complete TPMT deficiency Budesonide Usually none
Cosmetic changes (moon faces, acne and hirsutism) Cirrhosis Prednisone Osteoporosis
Emotional instability
Diabetes
Hypertension
Cosmetic changes (see budesonide)
Cataracts
Weight gain Vertebral compression
Psychosis
Brittle diabetes
Uncontrolled hypertension TPMT = thiopurine methyltransferase. The treatment of AIH consists of 2 phases: 1) induction of remission and 2) maintenance of remission. Please refer to Table 5 for detailed treatment regimens in each phase. Table 5: Most Common Treatment Options for Autoimmune Hepatitis
Combination Treatment
Prednisone + Azathioprine Combination Treatment
Budesonide + Azathioprine Prednisone Monotherapy Induction Week 1 30 mg/d + 50 mg/d 9 mg/d + 50 mg/d Prednisone 60 mg/d Week 2 25 mg/d + 50 mg/d 9 mg/d + 50 mg/d Prednisone 40 mg/d Week 3 20 mg/d + 50 mg/d 6 mg/d + 50 mg/d Prednisone 30 mg/d Week 4 15 mg/d + 50 mg/d 6 mg/d + 50 mg/d Prednisone 20 mg/d Maintenance First 12 months Prednisone 10 mg/d + Azathioprine 50 mg/d Budesonide 6 mg/d + Azathioprine 50 mg/d Prednisone 20 mg/d or less for at least 24 months 12-24 months Prednisone taper 2.5 mg/week until withdrawal. Thereafter azathioprine monotherapy 50-100 mg/day Consider budesonide taper until withdrawal. Thereafter azathioprine monotherapy 50-100 mg/day
Treatment Withdrawal
After 24 months of complete remission
OR
Liver biopsy showing absence of inflammation Same Same Indication
Preferred over prednisone monotherapy as fewer side effects Potential frontline therapy
Patients with obesity, acne, diabetes, and hypertension may benefit Reserved for patients who cannot take azathioprine Disadvantages
Side effects of prednisone, although less often and less severe than high-dose prednisone Expensive
Fewer studies showing efficacy Severe corticosteroid induced side effects Induction Phase In the induction phase, prednisone 30 mg per day plus azathioprine 50 mg per day is started for 1 week. This is followed by a prednisone taper over the course of 4 weeks with a fixed azathioprine dose of 50 mg per day to achieve a dose of prednisone 10 mg per day plus azathioprine 50 mg per day as shown in Table 5. Should budesonide plus azathioprine be selected, induction is achieved with combination of budesonide 3 mg three times daily plus azathioprine 50 mg per day for 2 weeks, followed by a budesonide 3 mg twice daily thereafter. Maintenance Phase For those receiving prednisone plus azathioprine, maintenance phase begins typically after 4 weeks, when the dose of prednisone 10 mg per day plus azathioprine 50 mg per day is started. This dose is continued for at least 1 full year. The daily maintenance dose of prednisone should remained fixed, as dose titration according to liver transaminases or alternate day schedules of prednisone are associated with incomplete histological improvement despite laboratory improvement. After 1 year of controlled disease, consideration can be given to withdrawal of prednisone while continuing azathioprine. Thereafter azathioprine monotherapy is continued for long-term maintenance. Patients can often be maintained on doses of azathioprine monotherapy of 50 mg per day to 100 mg per day with normal liver enzymes. Azathioprine doses of less than 100 mg per day have the advantage of less toxicity, particularly less leukopenia. Table 5 shows the medical regimen for AIH. If budesonide is used, the maintenance dose is 6 mg twice daily in combination with azathioprine 50 mg per day. One may consider tapering budesonide while maintaining azathioprine 50 mg per day to 100 mg per day (azathioprine monotherapy) after 12 months, but there are currently no studies on the long term effect of azathioprine monotherapy after budesonide plus azathioprine combination.