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新生Balb/c小鼠脑细胞上柯萨奇病毒B3的受体蛋白在免疫学上与HeLa细胞上的受体蛋白不同。

Receptor proteins on newborn Balb/c mouse brain cells for coxsackievirus B3 are immunologically distinct from those on HeLa cells.

作者信息

Xu R, Mohanty J G, Crowell R L

机构信息

Department of Microbiology and Immunology, Hahnemann University, Philadelphia, PA 19102-1192, USA.

出版信息

Virus Res. 1995 Mar;35(3):323-40. doi: 10.1016/0168-1702(94)00100-q.

Abstract

Newborn Balb/c mice are highly susceptible to infection by the six coxsackievirus serotypes of group B (CVB) and it is known that receptor for these viruses are in highest concentration in the brain as compared to other tissues. Therefore, proteins from the brain tissues of these animals were solubilized (Brain-Ext) and characterized for the identification of mouse brain receptor (MBR) proteins. Virus-blot analyses of Brain-Ext suggested that each of three virus variants of CVB3-(N, W and RD) recognized four receptor proteins designated p46, p44, p36 and p33 according to their molecular size. Similar analyses of cultured neurons from newborn Balb/c mice revealed the presence of the same four receptor proteins, while astrocytes appeared to possess only p46 and/or p44. Isoelectric focusing of Brain-Ext, focused MBR proteins in the pH range 4.0-8.5, with a peak around pH 5.7. P46 was found to be neuraminidase sensitive. A polyclonal rat antiserum (anti-MBR) protected cultured neurons and astrocytes against infection by CVB3, inhibited virus binding to these cells and recognized the same four receptor proteins on western-blots as detected on virus-blots by CVB3. However, a rabbit polyclonal anti-HeLa cell antiserum, which strongly binds to HeLa cells and protects them from CVB3 infection, neither recognized any of the receptor proteins in western-blot analyses of Brain-Ext nor inhibited CVB3 infection on cultured neurons and astrocytes. Conversely, anti-MBR did not recognize any of the receptor proteins by western-blot analysis of HeLa cell extracts nor did it inhibit CVB3 infection of HeLa cells.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

新生的Balb/c小鼠对B组六种柯萨奇病毒血清型(CVB)的感染高度敏感,并且已知与其他组织相比,这些病毒的受体在大脑中的浓度最高。因此,将这些动物脑组织中的蛋白质溶解(脑提取物)并进行表征,以鉴定小鼠脑受体(MBR)蛋白。对脑提取物进行病毒印迹分析表明,CVB3的三种病毒变体(N、W和RD)中的每一种都识别出四种受体蛋白,根据其分子大小分别命名为p46、p44、p36和p33。对新生Balb/c小鼠培养的神经元进行的类似分析显示存在相同的四种受体蛋白,而星形胶质细胞似乎仅具有p46和/或p44。脑提取物的等电聚焦将MBR蛋白聚焦在pH值4.0 - 8.5范围内,峰值约在pH 5.7。发现p46对神经氨酸酶敏感。一种多克隆大鼠抗血清(抗MBR)可保护培养的神经元和星形胶质细胞免受CVB3感染,抑制病毒与这些细胞的结合,并在蛋白质印迹上识别与CVB3在病毒印迹上检测到的相同的四种受体蛋白。然而,一种兔多克隆抗HeLa细胞抗血清,它能强烈结合HeLa细胞并保护它们免受CVB3感染,在对脑提取物的蛋白质印迹分析中既未识别出任何受体蛋白,也未抑制CVB3对培养的神经元和星形胶质细胞的感染。相反,抗MBR在对HeLa细胞提取物的蛋白质印迹分析中未识别出任何受体蛋白,也未抑制CVB3对HeLa细胞的感染。(摘要截断于250字)

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