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在受感染细胞和包膜病毒颗粒中鉴定由UL33编码的人巨细胞病毒G蛋白偶联受体同源物。

Identification of the human cytomegalovirus G protein-coupled receptor homologue encoded by UL33 in infected cells and enveloped virus particles.

作者信息

Margulies B J, Browne H, Gibson W

机构信息

Retrovirus Biology Laboratory, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

Virology. 1996 Nov 1;225(1):111-25. doi: 10.1006/viro.1996.0579.

DOI:10.1006/viro.1996.0579
PMID:8918538
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6953178/
Abstract

Human cytomegalovirus (HCMV), strain AD169, contains four genes (US27, US28, UL33, and UL78) that encode putative homologues of cellular G protein-coupled receptors (GCRs). GCRs transduce extracellular signals to alter intracellular processes, and there is evidence that HCMV may elicit such changes at early times following infection. The US27, US28, and UL33 genes are transcribed during infection, and the US28 gene product has been found to be a functional receptor for the beta-chemokine class of immune modulators. The US27, UL33, and UL78 gene products have not been described and we have concentrated on identifying the UL33 protein because it is the most highly conserved of the GCR homologues among the human beta and gamma herpesviruses. We report here cloning UL33 into a recombinant baculovirus (rBV) and expressing it in insect cells; constructing a mutant HCMV with a disrupted UL33 gene; and identifying the UL33 protein in HCMV-infected cells and virus particles. Our results demonstrate that the UL33 protein (i) is expressed as a approximately 36-kDa, heat-aggregatable protein in rBV-infected cells, (ii) is modified heterogeneously by asparagine-linked glycosylation and expressed as a > or = 58-kDa glycoprotein that is present in the region of the cytoplasmic inclusions in HCMV-infected fibroblasts, (iii) is present in virions and two other enveloped virus particles, and (iv) is not essential for growth of HCMV in human foreskin fibroblast cultures.

摘要

人巨细胞病毒(HCMV)AD169株包含四个基因(US27、US28、UL33和UL78),这些基因编码细胞G蛋白偶联受体(GCR)的假定同源物。GCR转导细胞外信号以改变细胞内过程,并且有证据表明HCMV可能在感染后的早期引发此类变化。US27、US28和UL33基因在感染期间转录,并且已发现US28基因产物是免疫调节剂β趋化因子类的功能性受体。US27、UL33和UL78基因产物尚未见报道,我们专注于鉴定UL33蛋白,因为它是人类β和γ疱疹病毒中GCR同源物中保守性最高的。我们在此报告将UL33克隆到重组杆状病毒(rBV)中并在昆虫细胞中表达;构建具有破坏的UL33基因的突变型HCMV;以及在HCMV感染的细胞和病毒颗粒中鉴定UL33蛋白。我们的结果表明,UL33蛋白(i)在rBV感染的细胞中表达为约36 kDa的热聚集蛋白,(ii)通过天冬酰胺连接的糖基化进行异质性修饰,并表达为≥58 kDa的糖蛋白,该糖蛋白存在于HCMV感染的成纤维细胞的胞质内含物区域,(iii)存在于病毒粒子和其他两种包膜病毒颗粒中,并且(iv)对于HCMV在人包皮成纤维细胞培养物中的生长不是必需的。