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Hepatitis

Hepatitis is a gastroenterological disease, featuring inflammation of the liver. The clinical signs and prognosis, as well as the therapy, depend on the cause. more...

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Signs and symptoms

Hepatitis is characterised by fatigue, malaise, joint aches, abdominal pain, vomiting 2-3 times per day for the first 5 days, loss of appetite, dark urine, fever, hepatomegaly (enlarged liver) and jaundice (icterus). Some chronic forms of hepatitis show very few of these signs and only present when the longstanding inflammation has led to the replacement of liver cells by connective tissue; the result is cirrhosis. Certain liver function tests can also indicate hepatitis.

Types of hepatitis

Viral

Most cases of acute hepatitis are due to viral infections:

  • Hepatitis A
  • Hepatitis B
  • Hepatitis C
  • D-agent (requires presence of the hepatitis B virus)
  • Hepatitis E
  • Hepatitis F (discredited)
  • Hepatitis G
Please see the respective articles for more detailed information

Hepatitis A

Hepatitis A is an enterovirus transmitted by the orofecal route, such as contaminated food. It causes an acute form of hepatitis and does not have a chronic stage. The patient's immune system makes antibodies against Hepatitis A that confer immunity against future infection. People with Hepatitis A are usually advised to rest, stay hydrated and avoid alcohol. A vaccine is available that will prevent infection from hepatitis A for life.

Hepatitis B

Hepatitis B causes both acute and chronic hepatitis in some patients who are unable to eliminate the virus. Identified methods of transmission include blood (blood transfusion, now rare), tattoos (both amateur and professionally done), sexually or vertically (from mother to her unborn child). However, in about half of cases the source of infection cannot be determined. Blood contact can occur by sharing syringes in intravenous drug use, shaving accessories such as razor blades, or touching wounds on infected persons. Needle-exchange programmes have been created in many countries as a form of prevention. In the United States, 95% of patients clear their infection and develop antibodies against Hepatitis B virus. 5% of patients do not clear the infection and develop chronic infection; only these people are at risk of long term complications of Hepatitis B. Patients with chronic hepatitis B have antibodies against Hepatitis B, but these antibodies are not enough to clear the infection that establishes itself in the DNA of the affected liver cells. The continued production of virus combined with antibodies is a likely cause of immune complex disease seen in these patients. A vaccine is available that will prevent infection from hepatitis B for life. Hepatitis B infections result in 500,000 to 1,200,000 deaths per year worldwide due to the complications of chronic hepatitis, cirrhosis, and hepatocellular carcinoma. Hepatitis B is endemic in a number of (mainly South-East Asian) countries, making cirrhosis and hepatocellular carcinoma big killers. There are three, FDA-approved treatment options available for persons with a chronic hepatitis B infection: alpha-interferon, adefovir and lamivudine. In about 45% of persons on treatment achieve a sustained response.

Read more at Wikipedia.org


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Treatment of chronic hepatitis B infection
From American Family Physician, 10/15/05 by Anne D. Walling

Chronic hepatitis B infection can lead to cirrhosis, hepatic failure, and hepatocellular carcinoma. Current therapies are successful in a minority of patients. Approximately 19 percent of patients respond to interferon alfa, and 10 to 15 percent respond to lamivudine (Epivir). The long-term efficacy of current agents may be worse. For lamivudine, viral resistance is reported in more than one half of patients within three years. Janssen and colleagues reasoned that the combination of interferon alfa and lamivudine in a long-term treatment regimen could improve sustained response rates in chronic hepatitis B infection.

The authors conducted a randomized, double-blind controlled trial at 42 centers in 15 countries to compare the safety and effectiveness of interferon alfa monotherapy with combination therapy using interferon alfa plus lamivudine. Participants were at least 16 years of age and had been positive for hepatitis B surface antigen for at least six months. In the eight weeks before randomization, participants were required to be positive for hepatitis B e antigen (HBeAg) on at least two occasions and to have two documented measurements of alanine transaminase levels that were at least twice the upper limit of the normal range. Patients were excluded from the study if they had antibodies against hepatitis C or D viruses or if they were positive for human immunodeficiency virus. Patients with a history of antiviral or immunosuppressive therapy within the previous six months; pregnancy or inadequate contraception in women; substance abuse; liver, thyroid, psychiatric, or serious medical conditions; and inadequate leucocyte, granulocyte, or platelet counts also were excluded. After screening, patients were randomly assigned to therapy with 100 mcg pegylated interferon alfa-2b once per week plus 100 mg lamivudine (combination therapy), or to monotherapy using 100 mcg pegylated alfa-2b weekly plus a daily placebo. After 32 weeks, the interferon dose in both groups was lowered to 50 mcg per week. Patients were monitored at outpatient clinics every four weeks during the 52 weeks of the study and for 26 weeks after treatment. In addition to monitoring of laboratory markers and reported adverse effects, participants underwent liver biopsy at the beginning of the study and were offered repeat biopsy after treatment.

Of the 307 patients randomized, 266 (87 percent) were included in the analysis. Reasons for exclusion included nonadherence with medication or follow-up visits, clearance of HBeAg before starting therapy, and problems in data verification from one study center. The patients in the two treatment groups were comparable at recruitment and at conclusion of the study. By the end of the 52 weeks, significantly more patients using combination therapy responded with loss of HBeAg (44 percent compared with 29 percent). However, by the end of the follow-up period (at 78 weeks), 35 percent of the combination therapy group and 36 percent of the monotherapy group had sustained response. This pattern was shown in two other markers of hepatitis B infection. Fibrosis scores improved in 33 percent of the 52 combination therapy patients who agreed to two biopsies, compared with 22 percent of the 58 patients assigned to monotherapy. Biopsies revealed deteriorating fibrosis scores in 38 percent of available patients in both treatment groups. Regardless of treatment group, the sustained response rate was significantly influenced by the hepatitis B virus genotype. For genotypes A and B, the sustained response rates were 47 and 44 percent, respectively. For genotypes C and D, the comparable rates were 28 and 25 percent. Side effects were common, especially influenza-like syndrome, which affected 62 to 74 percent of patients. Thirty-two serious adverse effects were reported, of which one half were attributed to therapy. Despite adverse effects, 91 percent of patients remained on therapy after the study.

The authors conclude that combination therapy was superior to monotherapy over 52 weeks, but this advantage was not sustained during follow-up. They emphasize that long-term use of lamivudine is contraindicated because of drug resistance, and that the virus genotype is a key predictor of response to antiviral therapy.

ANNE D. WALLING, M.D. Janssen HLA, et al. Pegylated interferon alfa-2b alone or in combination with lamivudine for HBeAg-positive chronic hepatitis B: a randomised trial. Lancet January 8, 2005;365:123-9.

COPYRIGHT 2005 American Academy of Family Physicians
COPYRIGHT 2005 Gale Group

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