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MTase Domain of Dendrolimus punctatus cypovirus VP3 Mediates Virion Attachment and Interacts with Host ALP Protein

机译:马尾松毛虫cypovirus VP3的MTase域介导病毒颗粒附着并与宿主ALP蛋白相互作用

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Dendrolimus punctatus cypovirus (DpCPV) is an important pathogen of D. punctatus , but little is known about the mechanisms of DpCPV infection. Here, we investigated the effects of VP3, VP4 and VP5 structural proteins on the viral invasion. Both the C-terminal of VP3 (methyltransferase (MTase) domain) and VP4 (A-spike) bound to Spodoptera exigua midgut brush border membrane vesicles (BBMVs) in a dose-dependent manner, and the binding was inhibited by purified DpCPV virions. Importantly, anti-MTase and anti-VP4 antibodies inhibited viral binding to S. exigua BBMVs. Using far-Western blots, a 65 kDa protein in Bombyx mori BBMVs, identified as alkaline phosphatase protein ( Bm ALP) by mass spectrometry, specifically interacted with DpCPV MTase. The interaction between MTase and Bm ALP was verified by co-immunoprecipitation in vitro. Pretreatment of B. mori BBMVs with an anti-ALP antibody or incubation of DpCPV virions with prokaryotically expressed Bm ALP reduced viral attachment. Additionally, Bm ALP inhibited DpCPV infection in S. exigua larvae. Our data provide evidence that the MTase domain and A-spike function as viral attachment proteins during the DpCPV infection process, and ALP is the ligand that interacts with DpCPV via the MTase domain. These results augment our understanding of the mechanisms used by cypoviruses to enter their hosts.
机译:马尾松毛虫cypovirus(DpCPV)是马尾松毛虫的重要病原体,但对DpCPV感染的机制知之甚少。在这里,我们调查了VP3,VP4和VP5结构蛋白对病毒侵袭的影响。 VP3(甲基转移酶(MTase)结构域)和VP4(A-spike)的C端均以剂量依赖的方式与斜纹夜蛾中肠刷缘膜囊泡(BBMV)结合,并且结合被纯化的DpCPV病毒体抑制。重要的是,抗MTase和抗VP4抗体抑制病毒与Exigua BBMV的结合。使用远Western印迹,家蚕BBMVs中的65 kDa蛋白通过质谱鉴定为碱性磷酸酶蛋白(Bm ALP),与DpCPV MTase特异性相互作用。 MTase和Bm ALP之间的相互作用通过体外共免疫沉淀进行了验证。用抗ALP抗体预处理家蚕双歧杆菌BBMV或将DpCPV病毒粒子与原核表达的Bm ALP孵育可减少病毒附着。此外,Bm ALP抑制了Exigua幼虫的DpCPV感染。我们的数据提供了证据,表明在DpCPV感染过程中MTase结构域和A-spike发挥病毒附着蛋白的作用,而ALP是通过MTase结构域与DpCPV相互作用的配体。这些结果加深了我们对杯状病毒进入其宿主的机制的理解。

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