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丙型流感病毒与人红细胞的附着

Attachment of influenza C virus to human erythrocytes.

作者信息

Nishimura H, Sugawara K, Kitame F, Nakamura K

机构信息

Department of Bacteriology, Yamagata University School of Medicine, Japan.

出版信息

J Gen Virol. 1988 Oct;69 ( Pt 10):2545-53. doi: 10.1099/0022-1317-69-10-2545.

Abstract

Binding experiments with radioactively labelled influenza C virions were carried out to investigate the interaction of the virus with human erythrocytes. The erythrocytes from any of 35 different individuals were found to contain influenza C virus-binding sites though their number was variable among the individuals and was much less than that on mouse, rat and chicken erythrocytes. Attachment of influenza C virus to human erythrocytes was inhibited completely by prior treatment of the virus with anti-HE monoclonal antibody having a strong haemagglutination inhibition activity. Pretreatment of erythrocytes with neuraminidase or the neuraminate-O-acetylesterase of influenza C virus resulted in a marked reduction in the level of virus binding. Thus it appears that human erythrocytes have a low level of O-acetylated sialic acid-containing glycoconjugates that can interact specifically with the HE glycoprotein of influenza C virus. Proteolytic digestion of erythrocytes with ficin, bromelain or V-8 protease inhibited virus binding almost completely, suggesting that the erythrocyte receptor for influenza C virus is a glycoprotein. In contrast to these enzymes, trypsin treatment of erythrocytes reduced virus binding by only about 50%, and alpha-chymotrypsin treatment did not inhibit at all. It was also found that treatment of erythrocytes with monoclonal antibody to the M or N blood group antigen greatly inhibited virus binding to the cells. These results, taken together, suggest that most influenza C virus receptors on human erythrocytes, if not all, reside on glycophorin A which is known to possess the M or N blood group activity.

摘要

进行了用放射性标记的丙型流感病毒粒子的结合实验,以研究该病毒与人红细胞的相互作用。发现来自35个不同个体中任何一个的红细胞都含有丙型流感病毒结合位点,尽管其数量在个体间存在差异,且远少于小鼠、大鼠和鸡红细胞上的结合位点。用具有强血凝抑制活性的抗HE单克隆抗体预先处理病毒,可完全抑制丙型流感病毒与人红细胞的附着。用神经氨酸酶或丙型流感病毒的神经氨酸-O-乙酰酯酶预先处理红细胞,会导致病毒结合水平显著降低。因此,似乎人红细胞具有低水平的含O-乙酰化唾液酸的糖缀合物,它们可与丙型流感病毒的HE糖蛋白特异性相互作用。用无花果蛋白酶、菠萝蛋白酶或V-8蛋白酶对红细胞进行蛋白水解消化几乎完全抑制病毒结合,这表明丙型流感病毒的红细胞受体是一种糖蛋白。与这些酶不同,用胰蛋白酶处理红细胞仅使病毒结合降低约50%,而用α-胰凝乳蛋白酶处理则根本不抑制。还发现用针对M或N血型抗原的单克隆抗体处理红细胞可极大地抑制病毒与细胞的结合。综合这些结果表明,人红细胞上的大多数(如果不是全部)丙型流感病毒受体存在于已知具有M或N血型活性的血型糖蛋白A上。

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