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B 亚群呼吸道合胞病毒附着蛋白的遗传多样性

Genetic diversity of the attachment protein of subgroup B respiratory syncytial viruses.

作者信息

Sullender W M, Mufson M A, Anderson L J, Wertz G W

机构信息

Department of Pediatrics, University of Alabama School of Medicine, Birmingham 35294-0011.

出版信息

J Virol. 1991 Oct;65(10):5425-34. doi: 10.1128/JVI.65.10.5425-5434.1991.

Abstract

Respiratory syncytial (RS) virus causes repeated infections throughout life. Between the two main antigenic subgroups of RS virus, there is antigenic variation in the attachment protein G. The antigenic differences between the subgroups appear to play a role in allowing repeated infections to occur. Antigenic differences also occur within subgroups; however, neither the extent of these differences nor their contributions to repeat infections are known. We report a molecular analysis of the extent of diversity within the subgroup B RS virus attachment protein genes of viruses isolated from children over a 30-year period. Amino acid sequence differences as high as 12% were observed in the ectodomains of the G proteins among the isolates, whereas the cytoplasmic and transmembrane domains were highly conserved. The changes in the G-protein ectodomain were localized to two areas on either side of a highly conserved region surrounding four cysteine residues. Strikingly, single-amino-acid coding changes generated by substitution mutations were not the only means by which change occurred. Changes also occurred by (i) substitutions that changed the available termination codons, resulting in proteins of various lengths, and (ii) a mutation introduced by a single nucleotide deletion and subsequent nucleotide insertion, which caused a shift in the open reading frame of the protein in comparison to the other G genes analyzed. Fifty-one percent of the G-gene nucleotide changes observed among the isolates resulted in amino acid coding changes in the G protein, indicating a selective pressure for change. Maximum-parsimony analysis demonstrated that distinct evolutionary lineages existed. These data show that sequence diversity exists among the G proteins within the subgroup B RS viruses, and this diversity may be important in the immunobiology of the RS viruses.

摘要

呼吸道合胞(RS)病毒可导致人一生反复感染。在RS病毒的两个主要抗原亚组之间,附着蛋白G存在抗原变异。亚组之间的抗原差异似乎在反复感染的发生中起作用。亚组内也存在抗原差异;然而,这些差异的程度及其对反复感染的作用尚不清楚。我们报告了对30年间从儿童中分离出的B亚组RS病毒附着蛋白基因多样性程度的分子分析。在分离株的G蛋白胞外域中观察到高达12%的氨基酸序列差异,而胞质和跨膜域高度保守。G蛋白胞外域的变化定位于围绕四个半胱氨酸残基的高度保守区域两侧的两个区域。引人注目的是,由替换突变产生的单氨基酸编码变化并非发生变化的唯一方式。变化还通过以下方式发生:(i)改变可用终止密码子的替换,导致产生各种长度的蛋白质;(ii)由单个核苷酸缺失和随后的核苷酸插入引入的突变,与分析的其他G基因相比,该突变导致蛋白质的开放阅读框发生移位。在分离株中观察到的G基因核苷酸变化中有51%导致G蛋白的氨基酸编码变化,表明存在变化的选择压力。最大简约分析表明存在不同的进化谱系。这些数据表明B亚组RS病毒的G蛋白之间存在序列多样性,这种多样性可能在RS病毒的免疫生物学中具有重要意义。

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