16, 17 With this limited genome, HCV replicates in hepatocytes by

16, 17 With this limited genome, HCV replicates in hepatocytes by relying on cellular systems, thereby co-opting cellular proteins in its life cycle. To date, HCV particles have been found to contain more than 10

host lipoproteins.11, 12 Incorporation of these host proteins into HCV virions may not be this website random, as other enveloped viruses selectively obtain host proteins. For example, HIV-1 selectively acquires more than 40 host proteins, but excludes some proteins such as CD4, CD45, CXCR4, CCR3, and CCR5, which are all highly expressed on HIV-1-infected cells.20 It is believed that HIV-1 acquires biologically functional RCA proteins during viral budding at the plasma membrane. HCV, however, may acquire CD59 while budding through the membranes of intracellular organelles rather than at the plasma membrane because HCV may exit the cells by way of a secretory pathway.21 FACS and western blot data in this study showed that human hepatocytes expressed high levels of intracellular and surface CD59 without a difference in their molecular weights (Fig. 1), thereby providing a possible

source for HCV to encounter and obtain CD59 in intracellular organelles such as the ER. Identifying these interactions is critical for understanding the life cycle of HCV, and may yield novel targets for development of therapeutic strategies. To date, abrogation of RCA function to regain antivirus Ab activity against enveloped viruses has only been selleck compound tested in vitro in artificial environments such as GVB systems.2, 5, 6, 8 These systems provide optimized conditions for complement activation in vitro, but have no clinical relevance because they do not adequately replicate in vivo conditions. In this study, CD59 blockers were directly added into patient plasma to abrogate the function of CD59 on the patient’s own viral particles,

resulting in destruction of primary virions. The enhanced virolysis was likely triggered by ADCML, as all six individuals chronically infected with HCV showed high titers of anti-E2 Abs and potent complement activity. ADCML efficacy, however, significantly varied among these samples, which may be affected by many factors including the nature of the host immune response, HCV virological features, and patient profiles, MCE公司 because they all affect the outcome of HCV infection. For example, HCV from patient Pt42 was one of the most resistant viruses to the ADCML. Accordingly, this patient had the lowest anti-HCV E2 Ab titer among all six patients examined. However, our sample size is too small to analyze the correlation between the Ab titer and virolysis. In addition, anti-HCV E1 Abs in plasma samples from these patients were not titrated. Thus, further investigations with large clinical samples are required to analyze the correlation of anti-HCV E1/E2 Ab titers and virolysis efficacy.

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