首页> 外文期刊>Archives of virology >Amino acid domains 280-297 of VP6 and 531-554 of VP4 are implicated in heat shock cognate protein hsc70-mediated rotavirus infection.
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Amino acid domains 280-297 of VP6 and 531-554 of VP4 are implicated in heat shock cognate protein hsc70-mediated rotavirus infection.

机译:VP6的氨基酸结构域280-297和VP4的531-554与热休克同源蛋白hsc70介导的轮状病毒感染有关。

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The rotavirus infection mechanism seems to be a multi-step process which is still not fully understood. The heat shock cognate protein hsc70 has been proposed as being a co-receptor molecule for rotavirus entry into susceptible cells. In this work, an attempt was made to determine the existence of possible domains for VP4 and VP6 binding to hsc70. We selected amino acid sequences 531-554 from VP4 and 280-297 from VP6 on the basis of already recognized sequences for binding to hsc70. This study determined that DLPs and synthetic peptides from VP6 (aa 280-297) and VP4 (aa 531-554), individually or in combination, inhibited rotavirus RRV, YM and WA entry into MA104 and Caco-2 cells in an additive and dose-dependent manner. Hyperimmune sera against these synthetic peptides blocked infection by infectious TLPs. Capture ELISA results showed that DLPs interact with hsc70, probably through VP6 as the specific interaction between hcs70 and DLPs was disrupted by a VP6 peptide. These results suggest that VP6 takes part during rotavirus cell entry by binding to hsc70. This, as well as previous work, provides insight concerning the function of hsc70 within a multi-step model of rotavirus entry.
机译:轮状病毒感染机制似乎是一个多步骤的过程,至今仍未完全了解。已经提出热休克同源蛋白hsc70是轮状病毒进入易感细胞的共受体分子。在这项工作中,尝试确定VP4和VP6与hsc70结合的可能域的存在。基于已经识别的与hsc70结合的序列,我们从VP4中选择了氨基酸序列531-554,从VP6中选择了氨基酸序列280-297。这项研究确定了VP6(aa 280-297)和VP4(aa 531-554)的DLP和合成肽单独或联合抑制轮状病毒RRV,YM和WA进入添加剂和剂量进入MA104和Caco-2细胞依赖的方式。针对这些合成肽的超免疫血清可阻止感染性TLP的感染。捕获ELISA结果显示DLP与hsc70可能通过VP6相互作用,因为hcs70与DLP之间的特异性相互作用被VP6肽破坏。这些结果表明VP6通过与hsc70结合而参与轮状病毒细胞进入。这以及以前的工作提供了有关hsc70在轮状病毒输入的多步骤模型中的功能的见解。

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