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Current Pharmaceutical Biotechnology

Editor-in-Chief

ISSN (Print): 1389-2010
ISSN (Online): 1873-4316

Mechanisms Involved in the Development of Chronic Hepatitis C as Potential Targets of Antiviral Therapy

Author(s): Paulina Jackowiak, Magdalena Figlerowicz, Anna Kurzynska-Kokorniak and Marek Figlerowicz

Volume 12, Issue 11, 2011

Page: [1774 - 1780] Pages: 7

DOI: 10.2174/138920111798377030

Price: $65

Abstract

At present, about 3% of the human population are infected with hepatitis C virus (HCV). The first, acute stage of the disease is usually asymptomatic. However, only 15-25% of the infected eliminate the virus, while the remaining patients develop chronic hepatitis C (CHC). After 10-30 years of CHC, cirrhosis occurs in 20-30% of patients; 5-10% of this group eventually suffer from hepatocellular carcinoma. Unfortunately, up till now no effective methods protecting against HCV or allowing for efficient CHC treatment have been elaborated. This is primarily because not much is known about the mechanism of CHC emergence and the factors affecting anti-HCV therapy. There are several lines of evidence that some specific features of the virus, especially its high genetic variability might be responsible for the maintenance of HCV infection. Moreover, a few mechanisms which affect host-virus interactions and can additionally support CHC development have recently been identified. Hybridization between the host-encoded, liver-specific microRNA (miR-122) and the 5-untranslated region of HCV genome was shown to be required for effective viral RNA replication. It was also postulated that HCV proteins mimic some of the human ones; that is why the virus is not eliminated. Another hypothesis assumes that interactions between HCV E2 glycoprotein and CD81 receptor modulate various cellular pathways, thus supporting viral propagation. There is no doubt that a better understanding of the mechanisms described above is of great importance for designing new therapeutic strategies and anti-HCV drugs.

Keywords: Antiviral therapy, CD81, chronic hepatitis C, genetic variability, HCV, miR-122, molecular mimicry, anti-HCV therapy, various cellular pathways, most prevalent human pathogens, anti-HCV drugs, several dermatological, High Genetic Variability, antisense oligonucleotides


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