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抗受体抗体与非靶细胞的结合使它们易于被细胞毒性T淋巴细胞克隆裂解。

Attachment of an anti-receptor antibody to non-target cells renders them susceptible to lysis by a clone of cytotoxic T lymphocytes.

作者信息

Kranz D M, Tonegawa S, Eisen H N

出版信息

Proc Natl Acad Sci U S A. 1984 Dec;81(24):7922-6. doi: 10.1073/pnas.81.24.7922.

Abstract

The molecular basis for the dependence of antigen recognition by T cells on products of the major histocompatibility complex (MHC) is unknown, and the antigenic structures that are actually bound by T-cell receptors are ill-defined. In this study, we asked whether a monoclonal antibody (mAb) that reacts with the T-cell receptor of a clone of murine cytotoxic T lymphocytes (CTL) and not with the receptors of other CTL clones can substitute for that clone's natural ligand in specific cytolytic reactions. To answer the question, a mAb (1B2) to the receptor of a CTL clone (2C) was attached covalently to 51Cr-labeled cells that were not otherwise susceptible to lysis by clone 2C, and the cells thus modified were then tested as targets for clone 2C and other CTL clones of similar specificity. All labeled cells modified in this way, including a murine cell line that expresses no cell-surface MHC class I molecules and a human cell line, were lysed by clone 2C but not by other CTL clones. If, however, instead of attaching the mAb to the receptor of clone 2C, the cells were modified by attaching to them mAbs to other surface antigens on CTL [lymphocyte function-associated antigen (LFA-1), Thy-1.2], they were not lysed. In cytolytic titrations, the cells that had been converted by attachment of mAb 1B2 into specific targets for clone 2C were just as susceptible to lysis by that clone as the clone's natural H-2d targets (e.g., P815 cells). However, some accessory surface molecules (LFA-1, Lyt-2) that are required for clone 2C to lyse its natural H-2d targets seemed not to be required for this clone to lyse the mAb-converted target cells. By demonstrating that a variety of different cell types can be thus converted into target cells for CTL, the approach described in this study may provide opportunities to analyze further the mechanisms by which CTL destroy target cells.

摘要

T细胞对抗原的识别依赖于主要组织相容性复合体(MHC)产物的分子基础尚不清楚,T细胞受体实际结合的抗原结构也尚不明确。在本研究中,我们探究了一种单克隆抗体(mAb)能否在特异性细胞溶解反应中替代克隆的天然配体,该单克隆抗体可与小鼠细胞毒性T淋巴细胞(CTL)克隆的T细胞受体发生反应,而不与其他CTL克隆的受体发生反应。为了回答这个问题,将针对CTL克隆(2C)受体的单克隆抗体(1B2)共价连接到51Cr标记的细胞上,这些细胞原本不易被克隆2C裂解,然后将如此修饰的细胞作为克隆2C和其他具有相似特异性的CTL克隆的靶细胞进行测试。所有以这种方式修饰的标记细胞,包括不表达细胞表面MHC I类分子的小鼠细胞系和人细胞系,均被克隆2C裂解,但未被其他CTL克隆裂解。然而,如果不是将单克隆抗体连接到克隆2C的受体上,而是通过将针对CTL上其他表面抗原[淋巴细胞功能相关抗原(LFA-1)、Thy-1.2]的单克隆抗体连接到细胞上来修饰细胞,那么这些细胞不会被裂解。在细胞溶解滴定中,通过连接单克隆抗体1B2而转化为克隆2C特异性靶细胞的细胞,与该克隆的天然H-2d靶细胞(如P815细胞)一样容易被该克隆裂解。然而,克隆2C裂解其天然H-2d靶细胞所需的一些辅助表面分子(LFA-1、Lyt-2),似乎并非该克隆裂解单克隆抗体转化的靶细胞所必需。通过证明多种不同类型的细胞可以因此转化为CTL的靶细胞,本研究中描述的方法可能为进一步分析CTL破坏靶细胞的机制提供机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec40/392265/ca8df88f617c/pnas00625-0262-a.jpg

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