Helen Devereux scite author profile

We have studied morbidity and mortality related to hepatitis C virus infection in haemophilic patients treated at our centre. 11/255 HCV seropositive patients have developed hepatic decompensation. 20 years after first exposure to lyophilized clotting factor concentrate the risk of hepatic decompensation is estimated to be 10.8% (95% CI 3.8-17.8%). There is a significantly increased risk associated with HIV infection, and also with increased age. For HIV seropositive patients the rates of decline in CD4 lymphocyte count and the development of p24 antigenaemia are significant risk factors for hepatic decompensation. Cirrhosis was seen in 9/19 HIV seropositive patients at post mortem. There was an association of cirrhosis with increased age but not with CD4 count, p24 antigenaemia, or AIDS. In conclusion, HCV infection is associated with serious liver disease in haemophilic patients, but so far this has been restricted to a minority of those at risk. HIV co-infection accelerates progression to hepatic decompensation, and we speculate that this is probably due to enhanced HCV replication in the presence of immune deficiency.

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Rapid decline in detectability of HIV-1 drug resistance mutations after stopping therapy

Devereux¹,

Youle²,

Johnson³

et al. 1999

AIDS

253

106

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Replicative fitness in vivo of HIV‐1 variants with multiple drug resistance‐associated mutations

Devereux¹,

Emery²,

Johnson³

et al. 2001

Journal of Medical Virology

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The relative fitness of HIV-1 viral variants containing a broad range of drug resistance-associated mutations has been little studied in vivo. Understanding the relative fitness associated with viruses containing mutations may aid future therapeutic management. The aim of this study was to investigate the relative fitness of mutant viruses by assessing a cohort of patients who had developed resistance to many drugs and subsequently stopped all therapy. Eleven patients were assessed for drug resistance associated mutations in the protease (PR) and reverse transcriptase (RT) genes before and, at multiple time points, after stopping therapy. Relative fitness was calculated as a function of the rate of disappearance of mutant viruses when therapy was stopped. The least fit viruses were associated with the RT mutation M184I/V (11.6% less fit) and the PR mutations D30N (12.4% less fit) and M46I/L (21% less fit). Mutations at these codons were associated with significant reductions in fitness levels compared to wild-type viruses. Mutations at codons 10, 20, 36, and 63 in the PR gene remained fairly constant when therapy was stopped and may not significantly reduce viral fitness. The rapid re-population of wild-type viruses may allow the recycling of antiretroviral drugs prescribed previously.

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Immunological, virological and clinical response to highly active antiretroviral therapy treatment regimens in a complete clinic population

Mocroft

Devereux²,

Kinloch-de-Loes³

et al. 2000

AIDS

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HCV RNA levels and HIV infection: evidence for a viral interaction in haemophilic patients

et al. 1994

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In order to investigate a possible interaction between HIV and HCV infections, we compared HCV RNA levels in 29 matched pairs of haemophilic patients seropositive for HCV and serodiscordant for HIV. Levels were assayed using the new Chiron Quantiplex bDNA assay and were found to be significantly higher in HIV seropositive patients. There was no association between HCV RNA and age, duration of HCV infection, concentrate usage, markers of HIV progression, or use of zidovudine. Our study supports the hypothesis that HIV infection facilitates HCV replication and leads to more severe liver damage.

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Helen Devereux

The progression of HCV‐associated liver disease in a cohort of haemophilic patients

Rapid decline in detectability of HIV-1 drug resistance mutations after stopping therapy

Replicative fitness in vivo of HIV‐1 variants with multiple drug resistance‐associated mutations

Immunological, virological and clinical response to highly active antiretroviral therapy treatment regimens in a complete clinic population

HCV RNA levels and HIV infection: evidence for a viral interaction in haemophilic patients

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