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药物处理的肿瘤变体上一种80 kDa表面抗原的鉴定及其免疫原性:与莫洛尼鼠白血病病毒糖蛋白70的关系

Identification and immunogenic properties of an 80-kDa surface antigen on a drug-treated tumor variant: relationship to MuLV gp70.

作者信息

Grohmann U, Ullrich S J, Mage M G, Appella E, Fioretti M C, Puccetti P, Romani L

机构信息

Department of Experimental Medicine and Biochemical Sciences, University of Perugia, Italy.

出版信息

Eur J Immunol. 1990 Mar;20(3):629-36. doi: 10.1002/eji.1830200325.

Abstract

Highly immunogenic tumor variants are generated by in vitro or in vivo treatment of L5178Y murine lymphoma cells with triazene derivatives. Most of these variants express new transplantation antigens which are not present on the original L5178Y tumor cells. In this study, a polyclonal syngeneic antiserum raised to one such variant (L5178Y/DTIC) was employed in immunoprecipitation studies of cell surface and metabolically labeled L5178Y/DTIC cells. One- and two-dimensional electrophoretic analyses of the immunoprecipitates detected a surface antigen of approximately 80 kDa. Additionally, a 45-kDa component was detected in the lysate of [35S]methionine-labeled cells. Anti-xenotropic MuLV gp70 serum precipitated material whose electrophoretic pattern was similar to that of the 80-kDa surface antigen. Sequential immunoprecipitation analysis revealed that the molecules reactive with the variant-specific antiserum were removed by the anti-xenotropic gp70 antibodies, whereas immunodepletion was only partial when the cell extract was first treated with the variant-specific antibodies. After Western blotting, the 80- and 45-kDa antigens precipitated by the variant-specific antibodies were injected intrasplenically into recipient mice. Only the animals sensitized with the 80-kDa antigen developed specific immunity to L5178Y/DTIC cells in that they displayed an increased frequency in CTL precursors (CTLp) to the variant cells. Sera from mice sensitized to the 80-kDa protein specifically inhibited the development of a primary CTL response to L5178Y/DTIC cells.

摘要

用三氮烯衍生物对L5178Y小鼠淋巴瘤细胞进行体外或体内处理,可产生高免疫原性肿瘤变体。这些变体中的大多数表达新的移植抗原,而这些抗原在原始的L5178Y肿瘤细胞上并不存在。在本研究中,一种针对此类变体(L5178Y/DTIC)产生的多克隆同基因抗血清被用于对细胞表面和经代谢标记的L5178Y/DTIC细胞进行免疫沉淀研究。对免疫沉淀物进行一维和二维电泳分析,检测到一种约80 kDa的表面抗原。此外,在[35S]甲硫氨酸标记细胞的裂解物中检测到一个45 kDa的成分。抗嗜异性MuLV gp70血清沉淀出的物质,其电泳图谱与80 kDa表面抗原的相似。顺序免疫沉淀分析表明,与变体特异性抗血清反应的分子被抗嗜异性gp70抗体去除,而当细胞提取物先用变体特异性抗体处理时,免疫耗竭只是部分的。Western印迹后,将变体特异性抗体沉淀的80 kDa和45 kDa抗原脾内注射到受体小鼠体内。只有用80 kDa抗原致敏的动物对L5178Y/DTIC细胞产生了特异性免疫,因为它们对变体细胞的CTL前体(CTLp)频率增加。对80 kDa蛋白致敏的小鼠血清特异性抑制了对L5178Y/DTIC细胞的原发性CTL反应的发展。

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