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大鼠细胞毒性T淋巴细胞的膜表型

Membrane phenotype of the rat cytotoxic T lymphocyte.

作者信息

Gilman S C, Rosenberg J S, Feldman J D

出版信息

J Immunol. 1982 Sep;129(3):1012-6.

PMID:6980913
Abstract

We have examined rat cytotoxic T lymphocytes for expression of W3/25, OX8, Ia, Thy-1 antigens, and Fc gamma receptors using an effector cell-target cell conjugate formation assay in conjunction with immunofluorescence techniques. Lymph node, spleen, and peritoneal exudate T cells from Lewis rats immunized with allogeneic BN tumor cells specifically bound to and lysed BN tumor targets and BN blast cells, but did not bind or lyse syngeneic Lewis sarcoma cells, Lewis blast cells, or Lou/M blast cells. The numbers of binding and cytotoxic T lymphocytes were greatest in peritoneal exudate cells of immunized rats, less in spleens, and least in lymph nodes. Seventy to 80% of the lymphocytes bound to tumor targets were OX8+ T lymphocytes; less than 12% expressed W3/25, Ia, Thy-1, or Fc gamma R. Moreover, only OX8+ T cells efficiently lysed the target cells to which they were bound. The membrane phenotype of rat cytotoxic T lymphocytes was: OX8+, W3/25-, Ia-, Thy-1, and Fc gamma R-. Monoclonal OX8 antibody did not inhibit target cell binding or subsequent lysis by effector T cells, and there was no diminution of target cell binding or cytotoxic activity when the OX8 antigen was shed from the cell surface before interaction with target cells. There was no preferential association of OX8 antigen at the interface between the effector and target cell. Thus, OX8 antigen marks a subset of rat T lymphocytes that are cytotoxic but the molecule appears not to play a functional role in the cytotoxic process.

摘要

我们使用效应细胞 - 靶细胞共轭形成试验结合免疫荧光技术,检测了大鼠细胞毒性T淋巴细胞中W3/25、OX8、Ia、Thy - 1抗原和Fcγ受体的表达。用同种异体BN肿瘤细胞免疫的Lewis大鼠的淋巴结、脾脏和腹腔渗出液T细胞特异性地结合并裂解BN肿瘤靶细胞和BN原始细胞,但不结合或裂解同基因的Lewis肉瘤细胞、Lewis原始细胞或Lou/M原始细胞。结合和具有细胞毒性的T淋巴细胞数量在免疫大鼠的腹腔渗出液细胞中最多,在脾脏中较少,在淋巴结中最少。与肿瘤靶细胞结合的淋巴细胞中,70%至80%是OX8 + T淋巴细胞;表达W3/25、Ia、Thy - 1或FcγR的细胞少于12%。此外,只有OX8 + T细胞能有效地裂解它们所结合的靶细胞。大鼠细胞毒性T淋巴细胞的膜表型为:OX8 +、W3/25 -、Ia -、Thy - 1和FcγR -。单克隆OX8抗体不抑制效应T细胞与靶细胞的结合或随后的裂解,并且在与靶细胞相互作用之前,当OX8抗原从细胞表面脱落时,靶细胞结合或细胞毒性活性没有降低。在效应细胞和靶细胞之间的界面处,OX8抗原没有优先结合。因此,OX8抗原标记了大鼠T淋巴细胞的一个具有细胞毒性的亚群,但该分子似乎在细胞毒性过程中不发挥功能作用。

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