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Folding of an MHC class II-restricted tumor antigen controls its antigenicity via MHC-guided processing.

机译:MHC II类限制性肿瘤抗原的折叠通过MHC指导的加工过程控制其抗原性。

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摘要

CD4(+) and CD8(+) T cell responses to endogenous retroviral envelope glycoprotein gp90 generate protective immunity to murine colon carcinoma CT26. A panel of I-A(d)-restricted T cell hybridomas recognize gp90 synthesized by CT26 cells but not by other gp90-expressing tumors. Here we report that antigenicity resides in an incompletely folded form of gp90 that is unique to CT26. In contrast to more compact forms of gp90 that are present in other tumors, this open conformer is captured by recycling I-A(d) on antigen-presenting cells and is processed intracellularly. Thus, gp90 acquires immunodominance via MHC-guided processing, and the generation of an MHC class II-restricted response can be controlled by the intracellular folding environment of antigen-expressing cells.
机译:CD4(+)和CD8(+)T细胞对内源性逆转录病毒包膜糖蛋白gp90的反应产生对鼠结肠癌CT26的保护性免疫。一组受I-A(d)限制的T细胞杂交瘤可识别CT26细胞合成的gp90,但不能识别其他表达gp90的肿瘤。在这里我们报告抗原性存在于gp90的不完全折叠形式中,这是CT26独有的。与存在于其他肿瘤中的gp90的更紧凑形式相反,这种开放的构象异构体通过在抗原呈递细胞上回收I-A(d)捕获并在细胞内加工。因此,gp90通过MHC指导的处理获得免疫优势,并且可以通过表达抗原的细胞的细胞内折叠环境来控制MHC II类限制性反应的产生。

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