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水泡性口炎病毒的唾液酸糖蛋白及其神经氨酸的细胞吸附功能。

Cellular adsorption function of the sialoglycoprotein of vesicular stomatitis virus and its neuraminic acid.

作者信息

Schloemer R H, Wagner R R

出版信息

J Virol. 1975 Apr;15(4):882-93. doi: 10.1128/JVI.15.4.882-893.1975.

Abstract

Exposure of vesicular stomatitis (VS) virions to neuraminidase resulted in loss of their ability to agglutinate goose erythrocytes and to attach to L cells concomitant with hydrolysis of sialic acid. These viral adsorptive functions were also destroyed by tryspsinization. Sialyl transferase resialylation in vitro of neuraminidase-treated VS virions restored their hamagglutinating and adsorptive functions almost to original levels. Erythrocyte and L cell receptors for attachment of VS virions were blocked by fully sialylated fetuin and by VS viral sialoglycopeptides. Smaller VS viral glycopeptides generated by extensive trypsinization were less effective inhibitors of hemagglutination than were larger glycopeptides; neuraminic acid and neuraminosyl lactose had no capacity to inhibit hamagglutination or adsorption of virus to L cells. These data suggest that cellular receptors for viral adsorption recognize sialoglycopeptides of a certain size. Neuraminidase desialylation did not significantly alter the isoelectric point of VS virions. Cells exposed to DEAE-dextran, trypsin, or neuraminidase showed significantly increased capacity to attach fully sialylated but not desialylated VS virions. Neuraminidase desialylation of L cells, Chinese hamster ovary cells, and Madin-Darby bovine kidney cells resulted in enhanced susceptibility to plaque formation by VS virus.

摘要

将水泡性口炎(VS)病毒粒子暴露于神经氨酸酶会导致其凝集鹅红细胞以及附着于L细胞的能力丧失,同时伴随着唾液酸的水解。这些病毒吸附功能也会因胰蛋白酶处理而被破坏。用唾液酸转移酶对经神经氨酸酶处理的VS病毒粒子进行体外再唾液酸化,几乎可将其血凝和吸附功能恢复至原始水平。VS病毒粒子附着的红细胞和L细胞受体被完全唾液酸化的胎球蛋白和VS病毒唾液糖肽所阻断。广泛胰蛋白酶处理产生的较小的VS病毒糖肽对血凝的抑制作用不如较大的糖肽有效;神经氨酸和神经氨酰乳糖没有抑制血凝或病毒吸附到L细胞的能力。这些数据表明,病毒吸附的细胞受体识别一定大小的唾液糖肽。神经氨酸酶去唾液酸化并没有显著改变VS病毒粒子的等电点。暴露于二乙氨基乙基葡聚糖、胰蛋白酶或神经氨酸酶的细胞显示出附着完全唾液酸化而非去唾液酸化的VS病毒粒子的能力显著增强。对L细胞、中国仓鼠卵巢细胞和马-达二氏牛肾细胞进行神经氨酸酶去唾液酸化会导致对VS病毒形成蚀斑的易感性增强。

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