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提交给第八届人类白细胞分化抗原研讨会的单克隆抗体对轮状病毒-细胞附着和进入的特异性及效果评估。

Evaluation of specificity and effects of monoclonal antibodies submitted to the Eighth Human Leucocyte Differentiation Antigen Workshop on rotavirus-cell attachment and entry.

作者信息

Halasz Peter, Fleming Fiona E, Coulson Barbara S

机构信息

Department of Microbiology and Immunology, The University of Melbourne, Vic. 3010, Australia.

出版信息

Cell Immunol. 2005 Jul-Aug;236(1-2):179-87. doi: 10.1016/j.cellimm.2005.08.025. Epub 2005 Oct 5.

DOI:10.1016/j.cellimm.2005.08.025
PMID:16169540
Abstract

Rotavirus infection of permissive cells is a multi-step process that requires interaction with several cell surface receptors. Integrins alpha2beta1, alpha4beta1, alphaXbeta2, and alphavbeta3 are involved in the attachment and entry into permissive cells for many rotavirus strains. However, possible roles of known partners of these integrins in this process have not been studied. Here, the specificities of new monoclonal antibodies directed to beta1 and beta2 integrins were determined using integrin-transfected cells. The ability of monoclonal antibodies to integrin partners CD82, CD151, CD321, and CD322 to bind rotavirus-permissive cell lines (MA104, Caco-2, and RD) and K562 cells expressing or lacking alpha4beta1 also was investigated. CD82 and CD151 were expressed on K562, alpha4-K562, and RD cells. CD321-specific antibodies bound K562, alpha4-K562, MA104, and Caco-2 cells. CD322 expression was detected on MA104 but not Caco-2 cells. Antibodies to CD82, CD151, CD321, and CD322 that bound these cells were investigated for their ability to inhibit cellular attachment and entry by rotaviruses. Antibody blockade of these integrin-associated proteins did not affect cell attachment or entry of the integrin-using rhesus rotavirus RRV or porcine rotavirus CRW-8, which uses alpha4beta1 integrin for infection. Antibody blockade of CD322 did not alter cell attachment or infectivity by human rotavirus strain RV-3, so RV-3 infection was independent of CD322. Overall, these studies indicate that CD82, CD151, CD321, and CD322 are unlikely to play a role in rotavirus-cell binding or entry.

摘要

轮状病毒感染允许性细胞是一个多步骤过程,需要与几种细胞表面受体相互作用。整合素α2β1、α4β1、αXβ2和αvβ3参与许多轮状病毒株对允许性细胞的附着和进入。然而,这些整合素已知配体在这一过程中的可能作用尚未得到研究。在这里,使用整合素转染细胞确定了针对β1和β2整合素的新型单克隆抗体的特异性。还研究了整合素配体CD82、CD151、CD321和CD322的单克隆抗体与轮状病毒允许性细胞系(MA104、Caco-2和RD)以及表达或缺乏α4β1的K562细胞结合的能力。CD82和CD151在K562、α4-K562和RD细胞上表达。CD321特异性抗体与K562、α4-K562、MA104和Caco-2细胞结合。在MA104细胞上检测到CD322表达,但在Caco-2细胞上未检测到。研究了与这些细胞结合的针对CD82、CD151、CD321和CD322的抗体抑制轮状病毒细胞附着和进入的能力。这些整合素相关蛋白的抗体阻断并不影响使用整合素的恒河猴轮状病毒RRV或使用α4β1整合素进行感染的猪轮状病毒CRW-8的细胞附着或进入。CD322的抗体阻断并未改变人轮状病毒株RV-3的细胞附着或感染性,因此RV-3感染与CD322无关。总体而言,这些研究表明CD82、CD151、CD321和CD322不太可能在轮状病毒与细胞的结合或进入中发挥作用。

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