The identified receptor tyrosine kinases (RTKs) mediate HCV this website entry by regulating CD81-claudin-1 coreceptor associations and viral glycoprotein-dependent membrane fusion. These results identify RTKs as previously unknown HCV entry cofactors and show that tyrosine kinase inhibitors have substantial antiviral activity. Inhibition of RTK function may constitute a new approach for prevention and treatment of HCV infection. The current standard of care for chronic hepatitis C virus (HCV) is a combination therapy of pegylated interferon alpha (PEG-IFN-α) and ribavirin. However, treatment success is highly genotype dependent, and, at best, only 50% of infected individuals show
a sustained virological
response. Dabrafenib solubility dmso The recent approval of direct antivirals targeting the HCV NS3/4A protease [e.g., telaprevir (Vertex Pharmaceuticals, Cambridge, MA) and boceprevir (Merck, Whitehouse Station, NJ)] will significantly change the landscape of treatment for HCV. However, the low genetic barrier to resistance of these compounds suggests that the generation of drug-resistant mutants will be significant, and, therefore, direct acting antivirals will need to be used in combination with PEG-IFN-α/ribavirin therapy. Thus, the race continues to develop safer, cheaper therapeutic strategies. Entry into the host cell is a critical event in the viral life cycle, and, as such, it represents a promising target for antiviral therapy. Indeed, this strategy has recently been approved for the treatment of
human immunodeficiency virus (HIV) infection, in which binding of the HIV gp120 to the cellular coreceptor, CCR5, is antagonized by maraviroc (Pfizer, New York, NY), resulting in a block of viral entry. However, the development of such strategies requires an in-depth knowledge of the viral-host interactions, leading to viral entry. Considerable progress of late has been made in defining how HCV enters human hepatocytes. HCV entry is a multistep process and involves the viral envelope glycoproteins and at least four critical host cell receptors that are essential for efficient HCV entry (see below), although the sequence of events and cellular signals involved 上海皓元医药股份有限公司 in the entry process remain unresolved. Exciting new work published in Nature Medicine by Lupberger et al. has identified receptor tyrosine kinases (RTKs) as playing a pivotal role in assisting HCV entry. This work adds significantly to our understanding of the HCV entry process. As a number of RTK inhibitors are approved for clinical use, this discovery may translate into novel therapeutic strategies to combat HCV infection. In recent years, there has been extensive investigation into elucidating the precise mechanisms of HCV entry into hepatocytes.