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与幼鼠腹泻相关的一种新型冠状病毒的血凝作用及结构多肽

Hemagglutination and structural polypeptides of a new coronavirus associated with diarrhea in infant mice.

作者信息

Sugiyama K, Amano Y

出版信息

Arch Virol. 1980;66(2):95-105. doi: 10.1007/BF01314978.

Abstract

The hemagglutination (HA) and receptor destroying enzyme (RDE) activities of a newly isolated mouse enteric coronavirus (designated as DVIM) are described. DVIM agglutinates mouse or rat red blood cells (RBC) at 4 degrees C. At 37 degrees C the agglutination was rapidly reversed. The optimal pH for HA and for RDE activities using mouse red cells were shown to be 6.5 and 7.3 respectively. Hemagglutination by DVIM was not inhibited by pretreatment of RBCs with Vibrio cholerae filtrate or by pretreatment with Influenza-A neuraminidase. Therefore, the DVIM receptors on RBCs differ from the receptors of Influenza-A, and the RDE activity of DVIM acts specifically on this receptor. In addition, an analysis of the DVIM polypeptides showed that the virions contain five major, VP1 (M.W. 139,000), VP2 (68,000), VP3 (53,000), VP4 (38,000), VP5 (22,000) and two minor, VP1a (110,000), VP1b (100,000) polypeptides. VP1 and VP1b were digested by bromelain, suggesting that they constitute the surface glycoproteins.

摘要

描述了一种新分离的小鼠肠道冠状病毒(命名为DVIM)的血凝(HA)和受体破坏酶(RDE)活性。DVIM在4℃时能凝集小鼠或大鼠红细胞(RBC)。在37℃时,凝集迅速逆转。使用小鼠红细胞时,HA和RDE活性的最佳pH值分别显示为6.5和7.3。用霍乱弧菌滤液预处理RBC或用甲型流感神经氨酸酶预处理,均不能抑制DVIM的血凝作用。因此,RBC上的DVIM受体与甲型流感的受体不同,DVIM的RDE活性特异性作用于该受体。此外,对DVIM多肽的分析表明,病毒粒子含有五种主要多肽,即VP1(分子量139,000)、VP2(68,000)、VP3(53,000)、VP4(38,000)、VP5(22,000)以及两种次要多肽,VP1a(110,000)、VP1b(100,000)。菠萝蛋白酶可消化VP1和VP1b,表明它们构成表面糖蛋白。

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