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人冠状病毒229E膜蛋白基因的序列分析。

Sequence analysis of the membrane protein gene of human coronavirus 229E.

作者信息

Jouvenne P, Richardson C D, Schreiber S S, Lai M M, Talbot P J

机构信息

Institut Armand-Frappier, Université du Québec, Laval, Canada.

出版信息

Virology. 1990 Feb;174(2):608-12. doi: 10.1016/0042-6822(90)90115-8.

Abstract

Human coronaviruses (HCV) are ubiquitous pathogens which cause respiratory, gastrointestinal, and possibly neurological disorders. To better understand the molecular biology of the prototype HCV-229E strain, the complete nucleotide sequence of the membrane protein (M) gene was determined from cloned cDNA. The open reading frame is preceded by a consensus transcriptional initiation sequence UCUAAACU, identical to the one found upstream of the N gene. The M gene encodes a 225-amino acid polypeptide with a molecular weight (MW) of 25,822, slightly higher than the apparent MW of 19,000-22,000 observed for the unprocessed M protein obtained after in vitro translation and immunoprecipitation. The M amino acid sequence presents a significant degree of homology (38%) with its counterpart of transmissible gastroenteritis coronavirus (TGEV). The M protein of HCV-229E is highly hydrophobic and its hydropathicity profile shows a transmembranous region composed of three major hydrophobic domains characteristic of a typical coronavirus M protein. About 10% (20 amino acids) of the HCV-229E M protein constitutes a hydrophilic and probably external portion. One N-glycosylation and three potential O-glycosylation sites are found in this exposed domain.

摘要

人冠状病毒(HCV)是普遍存在的病原体,可引起呼吸道、胃肠道以及可能的神经系统疾病。为了更好地理解原型HCV - 229E毒株的分子生物学,从克隆的cDNA中确定了膜蛋白(M)基因的完整核苷酸序列。开放阅读框之前是一个共有转录起始序列UCUAAACU,与在N基因上游发现的序列相同。M基因编码一个由225个氨基酸组成的多肽,分子量(MW)为25,822,略高于体外翻译和免疫沉淀后获得的未加工M蛋白观察到的19,000 - 22,000的表观分子量。M氨基酸序列与其对应的传染性胃肠炎冠状病毒(TGEV)具有显著程度的同源性(38%)。HCV - 229E的M蛋白具有高度疏水性,其亲水性图谱显示一个由典型冠状病毒M蛋白特有的三个主要疏水结构域组成的跨膜区域。HCV - 229E M蛋白约10%(20个氨基酸)构成一个亲水且可能位于外部的部分。在这个暴露区域发现了一个N - 糖基化位点和三个潜在的O - 糖基化位点。

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