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细胞毒性T细胞通过淋巴因子进行的抗原非依赖性激活。

Antigen-independent activation of cytotoxic T cells by lymphokines.

作者信息

Williams L D, McMaster W R, Teh H S

机构信息

Department of Microbiology, University of British Columbia, Vancouver, Canada.

出版信息

Immunology. 1988 May;64(1):121-8.

Abstract

Supernatants from phorbol myristate acetate (PMA)-stimulated EL4.IL2 cells (EL4.PMA), but not recombinant IL-2 (rIL-2), induced the production of cytotoxic T lymphocytes (CTL) in low density murine spleen cell cultures. CTL induction in these cultures was completely abrogated by treatment with anti-Thy-1 or anti-Lyt-2 antibody plus complement but not by anti-L3T4 antibody plus complement. Fractionation of EL4.PMA on a Sephadex G-150 column demonstrated that the CTL-inducing activity in EL4.PMA eluted with an apparent molecular weight of about 44,000 and was partially separated from IL-2. This 44,000 MW material was shown to contain insignificant amounts of PMA. Following a 3-day culture period with the partially purified factor, C57BL/6J thymocytes could proliferate and differentiate into cytotoxic cells in response to rIL-2, whereas there was no proliferation or generation of cytotoxic cells when the thymocytes were cultured in rIL-2 alone. The number of IL-2 receptor-positive cells in C57BL/6J thymocytes also increased from 1.1% to 22.8% after 3 days of culture in the partially purified factor. Recombinant IL-4 (BSF-1) and IL-5 (TRF), when used alone or in combination with rIL-2, were unable to induce a cytotoxic response under similar culture conditions. These findings are consistent with the interpretation that EL4.PMA contains a novel lymphokine that directly, or indirectly, induces the expression of IL-2 receptors on resting CTL precursors without intentional stimulation by specific antigen. In the presence of IL-2, these precursors may then differentiate into effector CTL.

摘要

佛波酯(PMA)刺激的EL4.IL2细胞(EL4.PMA)的培养上清液可诱导低密度小鼠脾细胞培养物中细胞毒性T淋巴细胞(CTL)的产生,但重组IL-2(rIL-2)则不能。用抗Thy-1或抗Lyt-2抗体加补体处理可完全消除这些培养物中的CTL诱导作用,但用抗L3T4抗体加补体处理则不能。在Sephadex G-150柱上对EL4.PMA进行分级分离表明,EL4.PMA中诱导CTL的活性以约44,000的表观分子量洗脱,并与IL-2部分分离。这种44,000 MW的物质显示含有少量的PMA。用部分纯化的因子培养3天后,C57BL/6J胸腺细胞可对rIL-2作出反应而增殖并分化为细胞毒性细胞,而当胸腺细胞仅在rIL-2中培养时则没有细胞毒性细胞的增殖或产生。在部分纯化的因子中培养3天后,C57BL/6J胸腺细胞中IL-2受体阳性细胞的数量也从1.1%增加到22.8%。重组IL-4(BSF-1)和IL-5(TRF)单独使用或与rIL-2联合使用时,在类似的培养条件下均不能诱导细胞毒性反应。这些发现与以下解释一致,即EL4.PMA含有一种新型淋巴因子,该因子直接或间接诱导静息CTL前体细胞上IL-2受体的表达,而无需特定抗原的有意刺激。在IL-2存在的情况下,这些前体细胞可能会分化为效应CTL。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ce06/1385196/624ca7702748/immunology00153-0120-a.jpg

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