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细胞毒性T淋巴细胞引发的靶细胞死亡:一种靶细胞突变体区分被动孔形成和主动细胞自杀机制。

Target cell death triggered by cytotoxic T lymphocytes: a target cell mutant distinguishes passive pore formation and active cell suicide mechanisms.

作者信息

Ucker D S, Wilson J D, Hebshi L D

机构信息

Division of Immunology, Medical Biology Institute, La Jolla, California 92037.

出版信息

Mol Cell Biol. 1994 Jan;14(1):427-36. doi: 10.1128/mcb.14.1.427-436.1994.

Abstract

The role of the target cell in its own death mediated by cytotoxic T lymphocytes (CTL) has been controversial. The ability of the pore-forming granule components of CTL to induce target cell death directly has been taken to suggest an essentially passive role for the target. This view of CTL-mediated killing ascribes to the target the single role of providing an antigenic stimulus to the CTL; this signal results in the vectoral degranulation and secretion of pore-forming elements onto the target. On the other hand, by a number of criteria, target cell death triggered by CTL appears fundamentally different from death resulting from membrane damage and osmotic lysis. CTL-triggered target cell death involves primary internal lesions of the target cell that reflect a physiological cell death process. Orderly nuclear disintegration, including lamin phosphorylation and solubilization, chromatin condensation, and genome digestion, are among the earliest events, preceding the loss of plasma membrane integrity. We have tested directly the involvement of the target cell in its own death by examining whether we could isolate mutants of target cells that have retained the ability to be recognized by and provide an antigenic stimulus to CTL while having lost the capacity to respond by dying. Here, we describe one such mutant, BW87. We have used this CTL-resistant mutant to analyze the mechanisms of CTL-triggered target cell death under a variety of conditions. The identification of a mutable target cell element essential for the cell death response to CTL provides genetic evidence that target cell death reflects an active cell suicide process similar to other physiological cell deaths.

摘要

细胞毒性T淋巴细胞(CTL)介导的靶细胞自身死亡的作用一直存在争议。CTL的成孔颗粒成分直接诱导靶细胞死亡的能力被认为表明靶细胞基本上处于被动角色。这种CTL介导杀伤的观点认为靶细胞的唯一作用是向CTL提供抗原刺激;该信号导致成孔元件的定向脱颗粒并分泌到靶细胞上。另一方面,根据一些标准,CTL触发的靶细胞死亡与膜损伤和渗透性裂解导致的死亡在根本上有所不同。CTL触发的靶细胞死亡涉及靶细胞的原发性内部损伤,这反映了一种生理性细胞死亡过程。有序的核解体,包括核纤层蛋白磷酸化和溶解、染色质浓缩以及基因组消化,是最早发生的事件之一,早于质膜完整性的丧失。我们通过检查是否能够分离出靶细胞突变体来直接测试靶细胞在其自身死亡中的作用,这些突变体保留了被CTL识别并提供抗原刺激的能力,但失去了通过死亡做出反应的能力。在此,我们描述了一个这样的突变体BW87。我们利用这个对CTL有抗性的突变体在各种条件下分析CTL触发的靶细胞死亡机制。鉴定出对CTL诱导的细胞死亡反应必不可少的可变靶细胞元件,提供了遗传学证据,表明靶细胞死亡反映了一种类似于其他生理性细胞死亡的主动细胞自杀过程。

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