H. Porst scite author profile

batches of anti-D immune globulin contaminated with hepatitis C virus (HCV) genotype 1b (20,000-480,000 copies/dose) from a single erythrocyte donor had been administered for prophylaxis of rhesus isoimmunization throughout East Germany. All 2,867 women involved had been recalled after January 12, 1979 for repeated screening of alanine transaminase (ALT). They were prospectively followed in regional centers. We have reexamined a cohort of 1,018 women (median age 24, range 16-38 years at infection) on follow-up for 20 years in 9 representative centers. Within 6 months after anti-D administration, 10% of these women had no evidence of disease and 90% had acute hepatitis C (n ‫؍‬ 917) including 49% with symptomatic and 22% with icteric course. After 20 years, 85% of the 917 affected women still tested positive for HCV antibodies (among them 3% responded to interferon treatment) and 55% were positive for HCV RNA (among them 7% were nonresponders to interferon and 3% were apparent HCV carriers). Only 4 (0.4%) had overt cirrhosis. Two (0.2%) died of superinfected fulminant hepatitis B or alcoholism and cirrhosis, respectively. Histology obtained in 44% of the viremic women showed hepatitis of minimal to moderate grade in 96%, portal fibrosis in 47%, and septal fibrosis in 3% of the cases.

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Outcome in a hepatitis C (genotype 1b) single source outbreak in Germany—a 25-year multicenter study

Wiese

Grüngreiff²,

Güthoff

et al. 2005

Journal of Hepatology

163

119

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Decreased immunogenicity of recombinant hepatitis B vaccine in chronic hepatitis C

Wiedmann¹,

Liebert²,

Oesen

et al. 2000

151

110

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The immunogenicity of hepatitis B vaccine is unknown for patients with chronic hepatitis C, although hepatitis B vaccination is highly recommended in these patients. We therefore studied in a prospective open trial of 59 patients with chronic hepatitis C (mean age 42 years, hepatitis C for G10 years, Child-Pugh score I5) and 58 healthy hospital staff persons the rate of nonresponse (anti-HBs F10 mIU/mL at 9 months) to recombinant hepatitis B vaccine (Gen H-B-Vax R ,10g intradeltoidal at month 0, 1, and 6). Nonresponse was observed in 18/59 (31%) patients with chronic hepatitis C and 5/58 (9%) healthy staff persons (P F .005) (vs. 7% in historical controls; P F .005), low response (anti-HBs 10-99 mIU/mL) in 19% of patients with chronic hepatitis C and 17% of staff persons. High-dose booster vaccination led to seroconversion in 12/15 (80%) of primary nonresponders. Primary nonresponse to HB vaccine was related neither to presence of early-stage liver cirrhosis nor magnitude of serum hepatitis C virus (HCV) RNA concentration, nor explained by the presence of human leukocyte antigen (HLA) types (B8 DR3, B44, DR7, DQ2) predisposing to low antibody response to hepatitis B surface antigen. The rate of primary nonresponse to the standard regimen of recombinant hepatitis B vaccine is surprisingly high in patients with longstanding chronic hepatitis C. Therefore, the antibody to HBV surface antigen (anti-HBs) titer response should be determined in these patients. Depending on the response titer, higher booster doses may be required to achieve and maintain seroprotection in these patients. (HEPATOLOGY 2000;31:230-234.)

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Transmission of hepatitis C virus to children and husbands by women infected with contaminated anti-D immunoglobulin

et al. 1995

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Improvement of Neurocognitive Function in Responders to an Antiviral Therapy for Chronic Hepatitis C

Kraus

Schäfer

Teuber

et al. 2013

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Earlier studies have suggested neurocognitive impairment in patients with chronic hepatitis C virus (HCV) infection even before liver cirrhosis has developed. Since these deficits might be reversible after successful antiviral therapy, we analyzed the long‐term course of neurocognitive parameters in HCV patients with and without successful virus elimination by an interferon‐based antiviral treatment. In a multicenter study including 168 HCV patients receiving antiviral therapy (peginterferon alpha‐2b and ribavirin) we performed a long‐term follow‐up of neurocognitive performance before and after treatment. Neurocognitive function was psychometrically assessed using the computer‐aided TAP (Test Battery of Attentional Performance). When tested at least 12 months after termination of antiviral treatment, patients with sustained virologic response (SVR) had improved significantly as compared to their pretreatment performance in three of five TAP subtasks (vigilance, P < 0.001; shared attention: optical task, P < 0.001; working memory, P < 0.001). Patients who failed to eradicate the virus, however, showed no significant long‐term changes in neurocognitive performance in all five subtasks assessed (0.194 < P < 0.804). In the posttreatment evaluation, neurocognitive function was significantly better in responders to the antiviral therapy as compared to nonresponders. Conclusion: Successful eradication of HCV leads to a significant improvement of relevant aspects of attentional and neurocognitive performance, indicating that the neurocognitive impairment caused by chronic HCV infection is potentially reversible. This therefore suggests an added therapeutic benefit of antiviral treatment in HCV infection. Improvement of neurocognitive function may be an additional treatment indication in patients with HCV. (HEPATOLOGY 2013;58:497–504)

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H. Porst

Low frequency of cirrhosis in a hepatitis C (genotype 1b) single-source outbreak in germany: A 20-year multicenter study

Outcome in a hepatitis C (genotype 1b) single source outbreak in Germany—a 25-year multicenter study

Decreased immunogenicity of recombinant hepatitis B vaccine in chronic hepatitis C

Transmission of hepatitis C virus to children and husbands by women infected with contaminated anti-D immunoglobulin

Improvement of Neurocognitive Function in Responders to an Antiviral Therapy for Chronic Hepatitis C

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