Kim Chonsaeng, Bergelson Jeffrey M
Division of Infectious Diseases, Children's Hospital of Philadelphia, Philadelphia, Pennsylvania, USA.
J Virol. 2014 Jan;88(1):434-43. doi: 10.1128/JVI.02706-13. Epub 2013 Oct 23.
Echovirus 7 enters polarized Caco-2 intestinal epithelial cells by a clathrin-mediated endocytic process and then moves through the endosomal system before releasing its genome into the cytoplasm. We examined the possible role in virus entry of core components of the autophagy machinery. We found that depletion of Beclin-1, Atg12, Atg14, Atg16, or LC3 with specific small interfering RNAs inhibited echovirus 7 infection upstream of uncoating but had little or no effect on virus attachment to the cell surface. These data indicate that multiple autophagy-related proteins are important for one or more events that occur after the virus has bound its receptor on the cell surface but before RNA is released from the virus capsid. Although we have not determined the mechanism by which each protein contributes to virus entry, we found that stable depletion of Atg16L1 interfered with virus internalization from the cell surface rather than with intracellular trafficking. Autophagy gene products may thus participate in the endocytic process that moves virus into polarized Caco-2 cells.
埃可病毒7通过网格蛋白介导的内吞过程进入极化的Caco-2肠上皮细胞,然后在内体系统中移动,最后将其基因组释放到细胞质中。我们研究了自噬机制的核心成分在病毒进入过程中可能发挥的作用。我们发现,用特异性小干扰RNA耗尽Beclin-1、Atg12、Atg14、Atg16或LC3会在脱壳上游抑制埃可病毒7感染,但对病毒附着于细胞表面几乎没有影响。这些数据表明,多种自噬相关蛋白对于病毒在细胞表面结合其受体后但RNA从病毒衣壳释放之前发生的一个或多个事件很重要。尽管我们尚未确定每种蛋白促进病毒进入的机制,但我们发现稳定耗尽Atg16L1会干扰病毒从细胞表面的内化,而不是细胞内运输。因此,自噬基因产物可能参与将病毒转运到极化Caco-2细胞中的内吞过程。
