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细胞毒性T细胞:Lyt表型及Lyt抗血清对杀伤活性的阻断作用。

Cytotoxic T cells: Lyt phenotype and blocking of killing activity by Lyt antisera.

作者信息

Nakayama E, Shiku H, Stockert E, Oettgen H F, Old L J

出版信息

Proc Natl Acad Sci U S A. 1979 Apr;76(4):1977-81. doi: 10.1073/pnas.76.4.1977.

Abstract

WE REEXAMINED TWO QUESTIONS CONCERNING LYT ANTIGENS OF CYTOTOXIC T CELLS OF THE MOUSE

is Lyt-1 antigen expressed on cytotoxic effector cells and can cytotoxicity be blocked by antibody to Lyt antigens in the absence of added complement? A 3-hr (51)Cr-release assay with splenic effector cells and leukemia or myeloma target cells was used to measure cell-mediated cytotoxicity. The cytotoxic activity of effector cells against allogeneic targets was abolished by exposure to Lyt-1, Lyt-2, or Lyt-3 antiserum and complement. Specificity was established by tests with C57BL/6 Lyt congenic mice and absorption studies with thymocytes. Similarly, the cytotoxicity of effector cells directed against semisyngeneic myeloma targets was reduced by Lyt-1, -2, or -3 antiserum and complement. Effector cell cytotoxicity against another semisyngeneic target was only marginally affected by Lyt-1 antiserum and complement, but was abolished by Lyt-2 or -3 antiserum and complement. It appears likely that cytotoxic T cells are a heterogeneous population with regard to Lyt-1 expression and that past studies indicating an apparent absence of Lyt-1 on cytotoxic T cells revealed a quantitative, not qualitative, feature of these cells. With regard to the activity of Lyt antisera in the absence of added complement, selective blocking of effector cell cytotoxicity for allogeneic and semisyngeneic targets was found with Lyt-2 and Lyt-3 antisera but not with Lyt-1 antiserum. The specificity of blocking was established by tests with Lyt congenic mice and absorption studies with thymocytes. With the exception of blocking by antisera to the H-2 haplotype expressed by the target cell, no effector cell blocking was observed with alloantisera or heteroantisera to a range of other cell surface molecules present on mouse lymphoid cells. One possibility to account for the selective blocking by Lyt-2 and Lyt-3 antisera is that Lyt-2,3 determinants on the surface of cytotoxic T cells have a close spatial relation to the T cell receptor.

摘要

我们重新审视了两个关于小鼠细胞毒性T细胞的Lyt抗原的问题:细胞毒性效应细胞上是否表达Lyt-1抗原,以及在不添加补体的情况下,细胞毒性是否会被抗Lyt抗原的抗体阻断?使用脾效应细胞与白血病或骨髓瘤靶细胞进行3小时的(51)铬释放试验来测量细胞介导的细胞毒性。效应细胞对同种异体靶细胞的细胞毒性活性通过暴露于Lyt-1、Lyt-2或Lyt-3抗血清和补体而被消除。通过使用C57BL/6 Lyt同源小鼠进行测试以及用胸腺细胞进行吸收研究来确定特异性。同样,针对半同种异体骨髓瘤靶细胞的效应细胞的细胞毒性通过Lyt-1、-2或-3抗血清和补体而降低。效应细胞对另一个半同种异体靶细胞的细胞毒性仅受到Lyt-1抗血清和补体的轻微影响,但被Lyt-2或-3抗血清和补体消除。细胞毒性T细胞在Lyt-1表达方面似乎是一个异质群体,过去表明细胞毒性T细胞表面明显不存在Lyt-1的研究揭示了这些细胞的一个定量而非定性特征。关于在不添加补体的情况下Lyt抗血清的活性,发现Lyt-2和Lyt-3抗血清可选择性阻断效应细胞对同种异体和半同种异体靶细胞的细胞毒性,而Lyt-1抗血清则不能。通过使用Lyt同源小鼠进行测试以及用胸腺细胞进行吸收研究来确定阻断的特异性。除了针对靶细胞表达的H-2单倍型的抗血清的阻断作用外,未观察到针对小鼠淋巴细胞上存在的一系列其他细胞表面分子的同种异体抗血清或异种抗血清对效应细胞的阻断作用。Lyt-2和Lyt-3抗血清选择性阻断的一种可能解释是,细胞毒性T细胞表面的Lyt-2,3决定簇与T细胞受体具有密切的空间关系。

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