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12 results on '"Dahari H"'

1. Very early prediction of response to HCV treatment with PEG-IFN-alfa-2a and ribavirin in HIV/HCV-coinfected patients.

Author

Araújo, E. S. A., Dahari, H., Neumann, A. U., de Paula Cavalheiro, N., Melo, C. E., de Melo, E. S., Layden, T. J., Cotler, S. J., and Barone, A. A.

Subjects
*HEPATITIS C virus, *HIV-positive persons, *INTERFERONS, *RIBAVIRIN, *VIROLOGY, *PREDICTION models, *GENETICS of virus diseases
Abstract

The objective of this study was to find very early viral kinetic markers to predict nonresponse to hepatitis C virus (HCV) therapy in a group of human immunodeficiency virus (HIV)/HCV-coinfected patients. Twenty-six patients (15 HCV genotype-1 and 11 genotype-3) were treated with a 48-week regimen of peginterferon-alfa-2a (PEG-IFN) (180 μg/week) and weight-based ribavirin (11 mg/kg/day). Samples were collected at baseline; 4, 8, 12, 18, 24, 30, 36 and 42 h; days 2, 3, 4, 7, 8, 15, 22, 29, 43 and 57 then weekly and monthly. Five patients discontinued treatment. Seven patients (27%) achieved a sustained virological response (SVR). Nadir HCV RNA levels were observed 1.6 ± 0.3 days after initiation of therapy, followed by a 0.3- to 12.9-fold viral rebound until the administration of the second dose of PEG-IFN, which were not associated with SVR or HCV genotype. A viral decline <1.19 log for genotype-1 and <0.97 log for genotype-3, 2 days after starting therapy, had a negative predictive value (NPV) of 100% for SVR. The day 2 virological response had a similar positive predictive value for SVR as a rapid virological response at week 4. In addition, a second-phase viral decline slope (i.e., measured from day 2 to 29) <0.3 log/week had a NPV = 100% for SVR. We conclude that first-phase viral decline at day 2 and second-phase viral decline slope (<0.3 log/week) are excellent predictors of nonresponse. Further studies are needed to validate these viral kinetic parameters as early on-treatment prognosticators of nonresponse in patients with HCV and HIV. [ABSTRACT FROM AUTHOR]

Published
2011
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5. A perspective on modelling hepatitis C virus infection J. Guedj et al. A perspective on modelling HCV infection.

Author

Guedj, J., Rong, L., Dahari, H., and Perelson, A. S.

Subjects
*HEPATITIS C virus, *RNA, *ANTIVIRAL agents, *DRUG resistance, *INTERFERONS, *RIBAVIRIN, *MATHEMATICAL models, *CLINICAL trials
Abstract

By mathematically describing early hepatitis C virus (HCV) RNA decay after initiation of interferon (IFN)-based antiviral therapy, crucial parameters of the in vivo viral kinetics have been estimated, such as the rate of production and clearance of free virus, and the rate of loss of infected cells. Furthermore, by suggesting mechanisms of action for IFN and ribavirin mathematical modelling has provided a means for evaluating and optimizing treatment strategies. Here, we review recent modelling developments for understanding complex viral kinetics patterns, such as triphasic HCV RNA declines and viral rebounds observed in patients treated with pegylated interferon and ribavirin. Moreover, we discuss new modelling approaches developed to interpret the viral kinetics observed in clinical trials with direct-acting antiviral agents, which induce a rapid decline of wild-type virus but also engender a higher risk for emergence of drug-resistant variants. Lastly, as in vitro systems have allowed a better characterization of the virus lifecycle, we discuss new modelling approaches that combine the intracellular and the extracellular viral dynamics. [ABSTRACT FROM AUTHOR]

Published
2010
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6. Hepatitis C virus dynamics and cellular gene expression in uPA- SCID chimeric mice with humanized livers during intravenous silibinin monotherapy.

Author

DebRoy, S., Hiraga, N., Imamura, M., Hayes, C. N., Akamatsu, S., Canini, L., Perelson, A. S., Pohl, R. T., Persiani, S., Uprichard, S. L., Tateno, C., Dahari, H., and Chayama, K.

Subjects
*HEPATITIS C virus, *SEVERE combined immunodeficiency, *GENE expression, *SILIBININ, *LABORATORY mice, *THERAPEUTICS
Abstract

Legalon SIL ( SIL) is a chemically hydrophilized version of silibinin, an extract of milk thistle ( Silybum marianum) seeds that has exhibited hepatoprotective and antiviral effectiveness against hepatitis C virus ( HCV) in patients leading to viral clearance in combination with ribavirin. To elucidate the incompletely understood mode of action of SIL against HCV, mathematical modelling of HCV kinetics and human hepatocyte gene expression studies were performed in uPA- SCID-chimeric mice with humanized livers. Chronically HCV-infected mice ( n = 15) were treated for 14 days with daily intravenous SIL at 469, 265 or 61.5 mg/kg. Serum HCV and human albumin ( hAlb) were measured frequently, and liver HCV RNA was analysed at days 3 and 14. Microarray analysis of human hepatocyte gene expression was performed at days 0, 3 and 14 of treatment. While hAlb remained constant, a biphasic viral decline in serum was observed consisting of a rapid 1st phase followed by a second slower phase (or plateau with the two lower SIL dosings). SIL effectiveness in blocking viral production was similar among dosing groups (median ε = 77%). However, the rate of HCV-infected hepatocyte decline, δ, was dose-dependent. Intracellular HCV RNA levels correlated ( r = 0.66, P = 0.01) with serum HCV RNA. Pathway analysis revealed increased anti-inflammatory and antiproliferative gene expression in human hepatocytes in SIL-treated mice. The results suggest that SIL could lead to a continuous second-phase viral decline, that is potentially viral clearance, in the absence of adaptive immune response along with increased anti-inflammatory and antiproliferative gene expression in human hepatocytes. [ABSTRACT FROM AUTHOR]

Published
2016
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7. Dose-dependent decrease in hepatitis delta virus (HDV) RNA achieved with the oral prenylation inhibitor lonafarnib in a proof-of-concept, randomised, double-blinded, placebo-controlled study in patients with chronic HDV infection.

Author

Koh, C., Canini, L., Dahari, H., Cooper, S., Cory, D., Winters, M.A., Choong, I., Cotler, S.J., Kleiner, D.E., Yurdaydin, C., Heller, T., and Glenn, J.S.

Subjects
*HEPATITIS D virus, *DRUG dosage, *ISOPRENYLATION, *CLINICAL trials, *ORAL drug administration, *HEPATITIS treatment
Published
2015
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8. Cover Image.

Author

DebRoy, S., Hiraga, N., Imamura, M., Hayes, C. N., Akamatsu, S., Canini, L., Perelson, A. S., Pohl, R. T., Persiani, S., Uprichard, S. L., Tateno, C., Dahari, H., and Chayama, K.

Subjects
*VIRAL hepatitis, *PERIODICAL publishing, *PUBLICATIONS
Abstract

The cover image, by Kazuaki Chayama et al., is based on the Original Article Hepatitis C virus dynamics and cellular gene expression in uPA‐SCID chimeric mice with humanized livers during intravenous silibinin monotherapy, DOI: 10.1111/jvh.12551. [ABSTRACT FROM AUTHOR]

Published
2016
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9. LP36 : Understanding hepatitis delta virus and HBsAG kinetics during treatment with prenylation inhibitor lonafarnib via mathematical modeling.

Author

Canini, L., Koh, C., Cotler, S.J., Zhao, X., Uprichard, S.L., Haynes-Williams, V., Winters, M.A., Subramanya, G., Cooper, S.L., Pinto, P., Wolff, E., Bishop, R., Than Han, M.A., Kleiner, D.E., Keskin, O., Idilman, R., Yurdaydin, C., Glenn, J.S., Heller, T., and Dahari, H.

Subjects
*HEPATITIS associated antigen, *ISOPRENYLATION, *HEPATITIS D virus, *FARNESYLTRANSFERASE, *ANTIVIRAL agents, *MATHEMATICAL models, *REGRESSION analysis, *HEPATITIS treatment
Published
2015
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