Department of Pediatrics, Lamb Center for Pediatric Research, D7235 MCN, Vanderbilt University School of Medicine, 1161 21st Avenue South, Nashville, TN 37232, USA.
J Virol. 2011 Apr;85(7):3203-13. doi: 10.1128/JVI.02056-10. Epub 2011 Jan 19.
Reovirus cell entry is initiated by viral attachment to cell surface glycans and junctional adhesion molecule A. Following receptor engagement, reovirus is internalized into cells by receptor-mediated endocytosis using a process dependent on β1 integrin. Endocytosed virions undergo stepwise disassembly catalyzed by cathepsin proteases, followed by endosomal membrane penetration and delivery of transcriptionally active core particles into the cytoplasm. Cellular factors that mediate reovirus endocytosis are poorly defined. We found that both genistein, a broad-spectrum tyrosine kinase inhibitor, and PP2, a specific Src-family kinase inhibitor, diminish reovirus infectivity by blocking a cell entry step. Although neither inhibitor impedes internalization of reovirus virions, both inhibitors target virions to lysosomes. Reovirus colocalizes with Src during cell entry, and reovirus infection induces phosphorylation of Src at the activation residue, tyrosine 416. Diminished Src expression by RNA interference reduces reovirus infectivity, suggesting that Src is required for efficient reovirus entry. Collectively, these data provide evidence that Src kinase is an important mediator of signaling events that regulate the appropriate sorting of reovirus particles in the endocytic pathway for disassembly and cell entry.
呼肠孤病毒细胞进入是由病毒与细胞表面糖和连接黏附分子 A 的附着起始的。受体结合后,呼肠孤病毒通过受体介导的内吞作用被内吞进入细胞,该过程依赖于β1 整合素。内吞的病毒颗粒在组织蛋白酶蛋白酶的逐步催化作用下进行分步解体,随后进入内体膜并将转录活性的核心颗粒递送到细胞质中。介导呼肠孤病毒内吞作用的细胞因子尚未明确。我们发现,广泛的酪氨酸激酶抑制剂金雀异黄素和特定的Src 家族激酶抑制剂 PP2 通过阻断细胞进入步骤来降低呼肠孤病毒的感染力。虽然这两种抑制剂都不影响呼肠孤病毒颗粒的内化,但它们都将病毒颗粒靶向溶酶体。呼肠孤病毒在进入细胞时与Src 共定位,并且呼肠孤病毒感染诱导 Src 在激活残基酪氨酸 416 处磷酸化。通过 RNA 干扰减少 Src 的表达会降低呼肠孤病毒的感染力,这表明 Src 是呼肠孤病毒有效进入所必需的。总的来说,这些数据提供了证据表明 Src 激酶是调节呼肠孤病毒颗粒在细胞内吞途径中适当分拣以进行解体和细胞进入的信号事件的重要介质。
