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两株1型单纯疱疹病毒的糖蛋白C缺陷型突变体在极化或非极化细胞上表现出未改变的吸附特性。

Glycoprotein C-deficient mutants of two strains of herpes simplex virus type 1 exhibit unaltered adsorption characteristics on polarized or non-polarized cells.

作者信息

Griffiths A, Renfrey S, Minson T

机构信息

Department of Pathology, University of Cambridge, UK.

出版信息

J Gen Virol. 1998 Apr;79 ( Pt 4):807-12. doi: 10.1099/0022-1317-79-4-807.

Abstract

Mutants of herpes simplex virus type 1 (HSV-1) strain SC16, lacking each of the dispensable glycoproteins C, G, E, I or J, were examined for their ability to infect the apical or basolateral surfaces of polarized human epithelial cells. None of the mutants was significantly different from the wild-type parent when assayed on either surface. Since a previous report had demonstrated that glycoprotein C (gC) was necessary for the infection of apical surfaces of polarized epithelium, a second gC-negative mutant was constructed on a background of HSV-1 strain HFEM. This mutant displayed no phenotype when assayed on the apical surface. Furthermore, neither gC-negative mutant differed from its wild-type parent in its adsorption kinetics or specific infectivity on non-polarized Vero cells, a result which is inconsistent with the view that interactions between gC and cell surface proteoglycans constitute the initial adsorption process. Our findings thus conflict with previous reports and suggest that proposed functions of HSV-1 gC in the infection of polarized and non-polarized cells may be strain-dependent.

摘要

对单纯疱疹病毒1型(HSV-1)SC16株缺失可有可无的糖蛋白C、G、E、I或J的突变体进行检测,以观察它们感染极化人上皮细胞顶端或基底外侧表面的能力。在任一表面进行检测时,没有一个突变体与野生型亲本有显著差异。由于之前的一份报告表明糖蛋白C(gC)是感染极化上皮细胞顶端表面所必需的,因此在HSV-1 HFEM株的背景上构建了第二个gC阴性突变体。该突变体在顶端表面检测时没有表现出表型。此外,两个gC阴性突变体在非极化Vero细胞上的吸附动力学或比感染性方面与野生型亲本均无差异,这一结果与gC和细胞表面蛋白聚糖之间的相互作用构成初始吸附过程的观点不一致。因此,我们的发现与之前的报告相矛盾,并表明HSV-1 gC在极化和非极化细胞感染中所提出的功能可能具有毒株依赖性。

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