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确定CD21在B淋巴母细胞爱泼斯坦-巴尔病毒感染过程中的作用。

Determination of the role for CD21 during Epstein-Barr virus infection of B-lymphoblastoid cells.

作者信息

Martin D R, Marlowe R L, Ahearn J M

机构信息

Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

出版信息

J Virol. 1994 Aug;68(8):4716-26. doi: 10.1128/JVI.68.8.4716-4726.1994.

Abstract

Epstein-Barr virus (EBV), a herpesvirus with oncogenic potential, is camouflaged with glycoprotein 350/220, which mimics the human ligand C3dg and thereby binds to and exploits complement receptor type 2 (CR2; CD21), the EBV receptor. It has not been possible to determine the role of CR2 during postbinding events of viral infection because all B lymphocytes express endogenous CR2, precluding an informative study of receptor mutants. We have overcome this obstacle through creation of a novel experimental system based on molecular dissection of the ligand-binding domains of human CR2 and murine CR2. Our results demonstrate first, that two discontinuous amino acid substitutions within the ligand-binding domain of murine CR2 render it capable of mediating EBV infection of human B-lymphoblastoid cells, and second, that the specific role of CR2 during EBV infection is to capture virions at the cell surface, after which cofactors not associated with CR2 mediate postbinding events. These are the first studies to be described in which a cell that is normally susceptible to viral infection can be manipulated so as to direct entry of virions via recombinant or endogenous receptors.

摘要

爱泼斯坦-巴尔病毒(EBV)是一种具有致癌潜力的疱疹病毒,其表面覆盖有糖蛋白350/220,该糖蛋白模拟人类配体C3dg,从而与EBV受体补体受体2型(CR2;CD21)结合并利用它。由于所有B淋巴细胞都表达内源性CR2,因此无法确定CR2在病毒感染结合后事件中的作用,这使得对受体突变体的信息性研究无法进行。我们通过创建一种基于对人类CR2和小鼠CR2配体结合域进行分子剖析的新型实验系统克服了这一障碍。我们的结果首先表明,小鼠CR2配体结合域内的两个不连续氨基酸取代使其能够介导人类B淋巴母细胞的EBV感染,其次表明,CR2在EBV感染过程中的特定作用是在细胞表面捕获病毒粒子,之后与CR2无关的辅助因子介导结合后事件。这些是首次描述的研究,其中可以操纵正常易受病毒感染的细胞,以便通过重组或内源性受体引导病毒粒子进入。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0919/236411/bac79871b792/jvirol00017-0027-a.jpg

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