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流感病毒株选择性识别人类呼吸道上皮细胞上的唾液酸寡糖;宿主细胞在血凝素受体特异性选择中的作用。

Influenza virus strains selectively recognize sialyloligosaccharides on human respiratory epithelium; the role of the host cell in selection of hemagglutinin receptor specificity.

作者信息

Couceiro J N, Paulson J C, Baum L G

机构信息

Departamento Virologia, UFRJ, Brazil.

出版信息

Virus Res. 1993 Aug;29(2):155-65. doi: 10.1016/0168-1702(93)90056-s.

Abstract

The complement of sialyloligosaccharides present on the surface of human tracheal epithelium has been implicated as an important factor in the selection of hemagglutinin receptor specificity of human influenza A virus. Human strains of influenza A virus preferentially recognize host cell receptors bearing SA alpha 2,6Gal sequences, a sequence which is found on the surface of ciliated tracheal epithelium. A fluorescently-labelled H3 human virus strain bound avidly to the apical surface of human tracheal epithelium, while a fluorescently-labelled receptor variant strain, which preferentially binds SA alpha 2,3Gal sequences, showed little binding to the epithelial surface and localized primarily to intracellular mucin droplets. Extracts of human bronchial mucin, which is known to contain sialic acid primarily in the SA alpha 2,3Gal linkage, was a potent inhibitor of the binding of the receptor variant strain to trachea sections, while the binding of the parent strain was unaffected by the presence of mucin. Human bronchial mucin also inhibited the binding of the receptor variant strains, but not the parent virus strains, to human erythrocytes derivatized to contain SA alpha 2,6Gal sequences. These results suggest that a combination of selection pressures present in the respiratory tract environment have resulted in the evolution of a hemagglutinin receptor specificity in human influenza A virus strains which optimizes recognition of, binding to and infection of host cells.

摘要

人气管上皮表面存在的唾液酸寡糖的互补物被认为是人类甲型流感病毒血凝素受体特异性选择中的一个重要因素。甲型流感病毒的人源毒株优先识别带有SAα2,6Gal序列的宿主细胞受体,该序列存在于纤毛气管上皮表面。一种荧光标记的H3人病毒株与人类气管上皮的顶端表面紧密结合,而一种优先结合SAα2,3Gal序列的荧光标记受体变异株与上皮表面几乎没有结合,主要定位于细胞内粘蛋白滴。已知主要以SAα2,3Gal连接形式含有唾液酸的人支气管粘蛋白提取物是受体变异株与气管切片结合的有效抑制剂,而亲本毒株的结合不受粘蛋白存在的影响。人支气管粘蛋白也抑制受体变异株与衍生为含有SAα2,6Gal序列的人红细胞的结合,但不抑制亲本病毒株的结合。这些结果表明,呼吸道环境中存在的多种选择压力导致了甲型流感病毒人源毒株血凝素受体特异性的进化,从而优化了对宿主细胞的识别、结合和感染。

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