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麻疹病毒血凝素在自然进化及适应细胞培养过程中的序列差异

Sequence divergence of measles virus haemagglutinin during natural evolution and adaptation to cell culture.

作者信息

Rima B K, Earle J A, Baczko K, ter Meulen V, Liebert U G, Carstens C, Carabaña J, Caballero M, Celma M L, Fernandez-Muñoz R

机构信息

School of Biology and Biochemistry, The Queen's University of Belfast, UK.

出版信息

J Gen Virol. 1997 Jan;78 ( Pt 1):97-106. doi: 10.1099/0022-1317-78-1-97.

Abstract

Phylogenetic analysis of the sequence of the H gene of 75 measles virus (MV) strains (32 published and 43 new sequences) was carried out. The lineage groups described from comparison of the nucleotide sequences encoding the C-terminal regions of the N protein of MV were the same as those derived from the H gene sequences in almost all cases. The databases document a number of distinct genotype switches that have occurred in Madrid (Spain). Well-documented is the complete replacement of lineage group C2, the common European genotype at that time, with that of group D3 around the autumn of 1993. No further isolations of group C2 took place in Madrid after this time. The rate of mutation of the H gene sequences of MV genotype D3 circulating in Madrid from 1993 to 1996 was very low (5 x 10(-4) per annum for a given nucleotide position). This is an order of magnitude lower than the rates of mutation observed in the HN genes of human influenza A viruses. The ratio of expressed over silent mutations indicated that the divergence was not driven by immune selection in this gene. Variations in amino acid 117 of the H protein (F or L) may be related to the ability of some strains to haemagglutinate only in the presence of salt. Adaptation of MV to different primate cell types was associated with very small numbers of mutations in the H gene. The changes could not be predicted when virus previously grown in human B cell lines was adapted to monkey Vero cells. In contrast, rodent brain-adapted viruses displayed a lot of amino acid sequence variation from normal MV strains. There was no convincing evidence for recombination between MV genotypes.

摘要

对75株麻疹病毒(MV)毒株(32条已发表序列和43条新序列)的H基因序列进行了系统发育分析。从编码MV的N蛋白C端区域的核苷酸序列比较中得出的谱系组,在几乎所有情况下都与从H基因序列得出的谱系组相同。数据库记录了在西班牙马德里发生的一些明显的基因型转换。有充分记录的是,1993年秋季左右,当时常见的欧洲基因型C2谱系组被D3谱系组完全取代。此后在马德里没有再分离出C2谱系组。1993年至1996年在马德里流行的MV基因型D3的H基因序列的突变率非常低(给定核苷酸位置每年5×10⁻⁴)。这比在甲型人流感病毒的HN基因中观察到的突变率低一个数量级。表达突变与沉默突变的比率表明,该基因的差异不是由免疫选择驱动的。H蛋白第117位氨基酸(F或L)的变化可能与某些毒株仅在有盐存在时才能发生血凝的能力有关。MV对不同灵长类细胞类型的适应与H基因中非常少量的突变有关。当以前在人B细胞系中培养的病毒适应猴Vero细胞时,无法预测这些变化。相比之下,适应啮齿动物脑的病毒与正常MV毒株相比显示出大量氨基酸序列变异。没有令人信服的证据表明MV基因型之间发生了重组。

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