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人源和动物源H1流感病毒分离株的受体结合特性

Receptor binding properties of human and animal H1 influenza virus isolates.

作者信息

Rogers G N, D'Souza B L

机构信息

Department of Pharmacology, University of Iowa, College of Medicine, Iowa City 52242.

出版信息

Virology. 1989 Nov;173(1):317-22. doi: 10.1016/0042-6822(89)90249-3.

Abstract

It has been previously reported that several human H1 influenza viruses isolated prior to 1956, in contrast to human H3 isolates which are quite specific for SA alpha 2,6Gal sequences, apparently recognize both SA alpha 2,3Gal and SA alpha 2,6Gal sequences (Rogers, G.N., and Paulson, J.C., Virology 127, 361-373, 1983). In this report human H1 isolates representative of two epidemic periods, from 1934 to 1957 and from 1977 to 1986, and H1 influenza isolated from pigs, ducks, and turkeys were compared for their ability to utilize sialyloligosaccharide structures containing terminal SA alpha 2,3Gal or SA alpha 2,6Gal sequences as receptor determinants. Five of the eight human isolates from the first epidemic period recognize both SA alpha 2,3Gal and SA alpha 2,6Gal linkages, in agreement with our previous results. Of the remaining three strains, all isolated towards the end of the first epidemic, two appear to prefer SA alpha 2,6Gal sequences while the third preferentially binds SA alpha 2,3Gal sequences. In contrast to the early isolates, 11 of 13 human strains isolated during the second epidemic period preferentially bind SA alpha 2,6Gal containing oligosaccharides. On the basis of changes in receptor binding associated with continued passage in the laboratory for some of these later strains, it seems likely that human H1 isolates preferentially bind SA alpha 2,6Gal sequences in nature, and that acquisition of SA alpha 2,3Gal-binding is associated with laboratory passage. Influenza H1 viruses isolated from pigs were predominantly SA alpha 2,6Gal-specific while those isolated from ducks were primarily SA alpha 2,3Gal-specific. Thus, as has been previously reported for H3 influenza isolates, receptor specificity for influenza H1 viruses appears to be influenced by the species from which they were isolated, human isolates binding preferentially to SA alpha 2,6Gal-containing oligosaccharides while those isolated from ducks prefer SA alpha 2,3Gal-containing oligosaccharides. However, unlike the SA alpha 2,6Gal-specific H3 isolates, binding to cell surface receptors by the H1 influenza viruses is not sensitive to inhibition by horse serum glycoproteins, regardless of their receptor specificity. These results suggest that, while the H1 and H3 hemagglutinins appear to be subject to similar host-derived selective pressures, there appear to be certain fundamental differences in the detailed molecular interaction of the two hemagglutinins with their sialyloligosaccharide receptor determinants.

摘要

先前已有报道称,与对SAα2,6Gal序列具有高度特异性的人H3流感病毒分离株不同,1956年之前分离出的几种人H1流感病毒显然能识别SAα2,3Gal和SAα2,6Gal序列(Rogers, G.N., and Paulson, J.C., Virology 127, 361 - 373, 1983)。在本报告中,对代表两个流行时期(1934年至1957年以及1977年至1986年)的人H1分离株以及从猪、鸭和火鸡中分离出的H1流感病毒利用含有末端SAα2,3Gal或SAα2,6Gal序列的唾液酸寡糖结构作为受体决定簇的能力进行了比较。来自第一个流行时期的八个人类分离株中有五个能识别SAα2,3Gal和SAα2,6Gal连接,这与我们之前的结果一致。在其余三个均在第一个流行期接近尾声时分离出的毒株中,有两个似乎更倾向于SAα2,6Gal序列,而第三个则优先结合SAα2,3Gal序列。与早期分离株不同,在第二个流行期分离出的13个人类毒株中有11个优先结合含有SAα2,6Gal的寡糖。基于其中一些后期毒株在实验室连续传代后受体结合的变化,似乎人H1分离株在自然状态下优先结合SAα2,6Gal序列,而获得SAα2,3Gal结合能力与实验室传代有关。从猪中分离出的流感H1病毒主要对SAα2,6Gal具有特异性,而从鸭中分离出的则主要对SAα2,3Gal具有特异性。因此,正如先前关于H3流感分离株的报道一样,流感H1病毒的受体特异性似乎受其分离来源物种的影响,人分离株优先结合含有SAα2,6Gal的寡糖,而从鸭中分离出的则更喜欢含有SAα2,3Gal的寡糖。然而与对SAα2,6Gal具有特异性的H3分离株不同,无论其受体特异性如何,H1流感病毒与细胞表面受体的结合对马血清糖蛋白的抑制均不敏感。这些结果表明,虽然H1和H3血凝素似乎受到类似的宿主来源选择压力,但两种血凝素与其唾液酸寡糖受体决定簇的详细分子相互作用似乎存在某些根本差异。

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