Hemophilia A Clinical Trial
To determine the prevalence of hepatitis delta virus (HDV) in a large cohort of hemophiliacs and to elucidate the role of HDV in the development and progression of liver disease in this population.
BACKGROUND:
Patients with classical hemophilia (hemophilia A) and Christmas disease (hemophilia B) were
exposed to many hepatotropic viruses during the course of their therapy. Severe chronic
hepatitis among these patients was most likely related to persistent infection with
non-A,non-B hepatitis virus, hepatitis B virus, or delta hepatitis virus, a defective RNA
virus which is dependent upon coinfection with HBV for essential helper functions. Carriers
of HBV could contract an acute delta hepatitis infection that was invariably more severe than
the illness caused by HBV alone. The morbidity and mortality of delta hepatitis infection was
remarkably high. Transmission of the delta hepatitis agent appeared to follow the same routes
of transmission as HBV. Direct parenteral inoculation was the classic mode of transmission of
HBV which suggested a similar mode of transmission for delta hepatitis.
Hemophiliacs treated with commercial concentrates of coagulation factors prepared from pools
of plasma were at great risk to contract delta hepatitis infection. About 50 percent of these
patients had delta hepatitis virus antibodies. Also, studies of small cohorts indicated that
hepatitis delta infection was a major cause of chronic liver disease and cirrhosis.
Therefore, there was a critical need to evaluate the frequency and effect of hepatitis delta
infection in hemophiliacs in order to obtain data on the natural history of chronic liver
disease, comparing those with presumed chronic non-A,non-B hepatitis B alone, and combined
chronic delta and HBV infections.
This grant was awarded in response to a Request for Applications issued in 1986 on the
Prevalence and Consequences of Hepatitis Delta Infection in Hemophiliacs. The concept for the
initiative originated in the Blood Resources Working Group of the Blood Diseases and
Resources Advisory Committee and was approved by the National Heart, Lung, and Blood Advisory
Council in February 1985.
DESIGN NARRATIVE:
Both a prevalence study and a longitudinal study were conducted at several centers. In the
prevalence study, active hepatitis delta viral infection was established by non-invasive
serologic techniques such as hepatitis delta virus RNA/cDNA probes to detect hepatitis delta
virus RNA and an immunoblotting method to detect hepatitis delta antigen. These tests avoided
the need for liver biopsies to verify infection. In the longitudinal study, patients were
assigned to a core or auxiliary groups with those in the core group sampled every six months
for biochemical evidence of liver disease and those in the auxiliary group once a year.
Serogroups 0,3,5, and 6 and other participants with evidence of delta hepatitis infection
were assigned to the core group. Those patients who were immune to hepatitis B virus but were
anti-hepatitis delta virus positive were assigned two controls, matched by center, age, sex,
and hemophilia diagnosis and severity, from serogroups 5 who were without evidence of
hepatitis delta virus infection. Thus, the role of delta virus infection in liver disease in
hepatitis delta virus immune patients was evaluated. Follow-up continued for four years.
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