首页> 美国卫生研究院文献>Journal of Virology >Characterization of a protein found in cells infected with the spleen focus-forming virus that shares immunological cross-reactivity with the gp70 found in mink cell focus-inducing virus particles.
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Characterization of a protein found in cells infected with the spleen focus-forming virus that shares immunological cross-reactivity with the gp70 found in mink cell focus-inducing virus particles.

机译:在被脾脏聚焦形成病毒感染的细胞中发现的蛋白质的表征该蛋白与在貂细胞聚焦诱导病毒颗粒中发现的gp70具有免疫交叉反应。

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摘要

Previously we detected an antigen in cells infected with the spleen focus-forming virus (SFFV) with a radioimmunoassay specific for the gp 70's of murine leukemia mink cell focus-inducing (MCF) viruses. This antigen has now been characterized in competition radioimmunoassays with limiting dilutions of antibody and in pulse-labeling studies under conditions of antibody excess. Both methods of analysis indicate that the SFFV-encoded antigen is a glycoprotein with a molecular weight of approximately 52,000. The gp52 shared immunological reactivity and methionine-containing tryptic peptides with the gp70 of a Friend MCF virus and was expressed on the surface of SFFV-infected cells as well as in the cytoplasm. The gp52 could be detected (i) in fibroblastic cell lines from several species when these cells were infected with SFFV; (ii) in several established erythroleukemic cell lines; and (iii) in the spleens of mice recently infected with SFFV. Although it shared immunochemical properties with the gp70 of Friend MCF virus, the gp52 could be distinguished from the MCF gp70 (i) by its apparent lack of group and interspecies immunological determinants compared with MCF virus-derived gp70's; (ii) by its failure to be released from cells infected with SFFV or SFFV plus helper virus; (iii) by its molecular weight; and (iv) by tryptic peptide analysis. The results indicate that SFFV codes for an MCF gp70-related gp52 which is apparently no longer a virion structural protein like the MCF gp70 from which it was originally derived.
机译:以前,我们通过对小鼠白血病水貂细胞聚焦诱导(MCF)病毒gp 70特异的放射免疫分析,在感染了脾脏聚焦形成病毒(SFFV)的细胞中检测到抗原。现在已经在竞争性放射免疫分析中以有限的抗体稀释度和在抗体过量的条件下的脉冲标记研究中表征了这种抗原。两种分析方法均表明,SFFV编码的抗原是一种糖蛋白,分子量约为52,000。 gp52与Friend MCF病毒的gp70共享免疫反应性和含蛋氨酸的胰蛋白酶肽,并在感染SFFV的细胞表面以及细胞质中表达。 gp52可以被检测到(i)当几种细胞被SFFV感染后,它们在成纤维细胞中被检测到; (ii)在几种已建立的红白血病细胞系中; (iii)最近感染SFFV的小鼠的脾脏中。尽管gp52与Friend MCF病毒的gp70具有共同的免疫化学特性,但与MCF病毒衍生的gp70相比,它与MCF gp70(i)有明显区别,因为它明显缺乏基团和种间免疫学决定因子。 (ii)由于未能从感染了SFFV或SFFV加辅助病毒的细胞中释放出来; (iii)其分子量; (iv)通过胰蛋白酶肽分析。结果表明,SFFV编码与MCF gp70相关的gp52,而该gp52显然不再像最初源自其的MCF gp70一样,是病毒体结构蛋白。

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