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活化淋巴细胞对同种异体和异种靶细胞的细胞毒性差异。IV. 添加未标记细胞对靶细胞裂解的竞争性抑制

Differential cytotoxicity of activated lymphocytes on allogeneic and xenogeneic target cells. IV. Competitive inhibition of target cell lysis by addition of unlabeled cells.

作者信息

Stejskal V

出版信息

Scand J Immunol. 1976;5(5):479-86. doi: 10.1111/j.1365-3083.1976.tb00302.x.

Abstract

A competitive inhibition assay was used to define the specificity of the in vitro cytotoxicity of activated lymphocytes. Human and mouse effector cells were produced by prestimulation with phytohemagglutinin, pokeweed mitogen, or purified protein derivative for several days. The addition of increasing numbers of unlabeled Chang cells to a fixed number of stimulated human lymphocytes and 51Cr-labeled Chang cells gradually decreased chromium release. Admixture of unlabeled human bladder tumor cells, lung cells, or monkey kidney cells had a similar effect, whereas mouse L cells were not inhibitory. The reverse was found to be true when stimulated mouse lymphocytes and 51Cr-labeled mouse L cells were incubated. In this case, the addition of unlabeled L or rat tumor cells effectively inhibited 51Cr release, whereas human or monkey cells were less inhibitory. Both human and mouse cells inhibited the cytotoxicity of human effector lymphocytes towards mouse L cells. The cytotoxic effects of mouse lymphocytes on human cells were also decreased by addition of unlabeled human, monkey, or mouse cells, but in this case human cells were most inhibitory. The results indicate that activated lymphocytes recognize several surface structures on the target cells. Some of these structures may be shared by cells of different species origin, whereas others seem to be unique for cells from phylogenetically closely related species.

摘要

采用竞争性抑制试验来确定活化淋巴细胞体外细胞毒性的特异性。用人血细胞凝集素、商陆有丝分裂原或纯化蛋白衍生物预刺激人及小鼠效应细胞数天,以产生效应细胞。向固定数量的经刺激的人淋巴细胞和51Cr标记的Chang细胞中加入数量不断增加的未标记Chang细胞,可使铬释放逐渐减少。加入未标记的人膀胱肿瘤细胞、肺细胞或猴肾细胞也有类似效果,而小鼠L细胞则无抑制作用。当经刺激的小鼠淋巴细胞与51Cr标记的小鼠L细胞孵育时,情况则相反。此时,加入未标记的L细胞或大鼠肿瘤细胞可有效抑制51Cr释放,而人或猴细胞的抑制作用较弱。人和小鼠细胞均可抑制人效应淋巴细胞对小鼠L细胞的细胞毒性。加入未标记的人、猴或小鼠细胞也可降低小鼠淋巴细胞对人细胞的细胞毒性,但在这种情况下,人细胞的抑制作用最强。结果表明,活化淋巴细胞可识别靶细胞上的多种表面结构。其中一些结构可能为不同物种来源的细胞所共有,而另一些结构似乎是系统发育关系密切的物种的细胞所特有的。

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