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呼肠孤病毒3型与动物细胞上唾液酸化受体成分的差异相互作用。

Differential interaction of reovirus type 3 with sialylated receptor components on animal cells.

作者信息

Gentsch J R, Pacitti A F

机构信息

University of Pennsylvania, Department of Microbiology, School of Medicine, Philadelphia 19104-6076.

出版信息

Virology. 1987 Nov;161(1):245-8. doi: 10.1016/0042-6822(87)90192-9.

Abstract

In this report we study the interaction of reovirus type 3 Dearing (RV3) with vertebrate erythrocytes whose membrane glycoconjugates differ in the degree and position of O-acetylation of their sialic acid (NeuAc) residues. Binding to erythrocytes required the presence of NeuAc on cellular glycoconjugates, since pretreatment with sialidase (neuraminidase) abolished hemagglutination by RV3. Furthermore, we found that RV3 binds efficiently to and hemagglutinates all erythrocyte preparations possessing exclusively NeuAc, or a mixture of NeuAc and 4-O-acetyl-NeuAc (4-O-Ac-NeuAc), but poorly to erythrocytes bearing a mixture of 9-O-Ac-NeuAc and NeuAc, suggesting that RV3 binds preferentially to NeuAc-containing glycoconjugates. To gain further evidence for this hypothesis we treated chicken erythrocytes with influenza C virus neuraminate, 9-O-acetylesterase, to convert their 9-O-Ac-NeuAc residues to NeuAc. When hemagglutination assays were carried out on these cells, we observed a 16-fold increase in the hemagglutination titer for RV3 compared to untreated cells. When we treated bovine submaxillary mucin (BSM) with influenza C virus, we observed a dramatic increase in its potency as an inhibitor of RV3 hemagglutination. Concomitant with this, the 9-O-Ac-NeuAc residues on BSM were converted to NeuAc. Taken together and in conjunction with a previous report (A. F. Pacitti and J. R. Gentsch, 1987, J. Virol. 61 1407-1415), these results suggest that the virion attachment protein exhibits a strong preference for NeuAc over 9-O-Ac-NeuAc as a receptor component on erythrocytes.

摘要

在本报告中,我们研究了3型迪林呼肠孤病毒(RV3)与脊椎动物红细胞的相互作用,这些红细胞的膜糖缀合物在其唾液酸(NeuAc)残基的O-乙酰化程度和位置上有所不同。与红细胞的结合需要细胞糖缀合物上存在NeuAc,因为用唾液酸酶(神经氨酸酶)预处理可消除RV3的血凝作用。此外,我们发现RV3能有效结合并凝集所有仅含有NeuAc或NeuAc与4-O-乙酰基-NeuAc(4-O-Ac-NeuAc)混合物的红细胞制剂,但与含有9-O-乙酰基-NeuAc和NeuAc混合物的红细胞结合较差,这表明RV3优先结合含NeuAc的糖缀合物。为了进一步证明这一假设,我们用C型流感病毒神经氨酸9-O-乙酰酯酶处理鸡红细胞,将其9-O-Ac-NeuAc残基转化为NeuAc。对这些细胞进行血凝试验时,我们观察到与未处理细胞相比,RV3的血凝滴度增加了16倍。当我们用C型流感病毒处理牛颌下粘蛋白(BSM)时,我们观察到其作为RV3血凝抑制剂的效力显著增加。与此同时,BSM上的9-O-Ac-NeuAc残基被转化为NeuAc。综合这些结果并结合之前的一份报告(A. F. Pacitti和J. R. Gentsch,1987年,《病毒学杂志》61 1407 - 1415),这些结果表明,病毒体附着蛋白在红细胞上作为受体成分时,对NeuAc的偏好远高于9-O-Ac-NeuAc。

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