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白细胞介素-2成瘾:生长因子的撤除激活了依赖T细胞中的自杀程序。

IL-2 addiction: withdrawal of growth factor activates a suicide program in dependent T cells.

作者信息

Duke R C, Cohen J J

出版信息

Lymphokine Res. 1986 Fall;5(4):289-99.

PMID:2946903
Abstract

IL-2-dependent T effector cells usually die when deprived of growth factor. Cell death (as measured by plasma membrane breakdown) requires protein synthesis because it is inhibited by cycloheximide or emetine. When the DNA in several IL-2-dependent cell lines was examined following removal of IL-2, it was found that extensive chromatin cleavage precedes plasma membrane breakdown by several hours. The DNA fragments observed were not randomly generated but consisted of oligonucleosomes. This suggests that IL-2 deprivation led to activation of an endonuclease with specificity for linker DNA. DNA fragmentation, like cell death, did not occur in the presence of protein synthesis inhibitors. The protein(s) synthesized in response to IL-2 deprivation may, therefore, be the endonuclease or its activator; none of the IL-2-dependent T cells examined contain detectable endogenous endonuclease prior to IL-2 removal. DNA fragments were also found in vivo in lymph node cells draining a site of antigen administration. These results suggest that one aspect of the termination of immune responses involves activation of a cell suicide program in the expanded effector T cell clones. In this program an endonuclease is activated and chromatin is cleaved; as a result macromolecular synthesis begins to wind down so that repair synthesis stops; within a few hours, the cell lyses.

摘要

依赖白细胞介素-2的T效应细胞在缺乏生长因子时通常会死亡。细胞死亡(通过质膜破裂来衡量)需要蛋白质合成,因为它会被放线菌酮或依米丁抑制。在去除白细胞介素-2后检查几种依赖白细胞介素-2的细胞系中的DNA时发现,广泛的染色质裂解比质膜破裂提前数小时发生。观察到的DNA片段不是随机产生的,而是由寡核小体组成。这表明去除白细胞介素-2会导致对连接DNA具有特异性的核酸内切酶激活。与细胞死亡一样,在存在蛋白质合成抑制剂的情况下不会发生DNA片段化。因此,响应去除白细胞介素-2而合成的蛋白质可能是核酸内切酶或其激活剂;在去除白细胞介素-2之前,所检查的依赖白细胞介素-2的T细胞中没有一个含有可检测到的内源性核酸内切酶。在抗原注射部位引流的淋巴结细胞中也在体内发现了DNA片段。这些结果表明,免疫反应终止的一个方面涉及在扩增的效应T细胞克隆中激活细胞自杀程序。在这个程序中,核酸内切酶被激活,染色质被裂解;结果大分子合成开始逐渐减少,从而使修复合成停止;在几个小时内,细胞裂解。

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