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细胞毒性T淋巴细胞诱导靶细胞裂解的显微电影摄影和电子显微镜分析。

Microcinematographic and electron microscopic analysis of target cell lysis induced by cytotoxic T lymphocytes.

作者信息

Matter A

出版信息

Immunology. 1979 Feb;36(2):179-90.

Abstract

A study was carried out to determine the sequence of events of T-cell mediated target cell lysis in microcinematography and electron microscopy. Highly efficient cytotoxic T lymphocytes (CTL) were generated in vivo and in vitro using preimmunized spleen cells and purification procedures. Such CTL were highly specific. This specificity correlated well with the number of adhesions formed between CTL and targets and this criterion was used to study killer-target cell interaction. Microcinematography showed that target cell lysis at the single cell level, despite time variations, could be clearly separated into three phases: (a) a recognition phase, visible by random crawling of CTL over the target cell surface until firm contact was established; (b) a post-recognition phase, during which firm contact between CTL and target was maintained without gross modification of either cell; (c) a phase of target cell disintegration, mainly characterized by vigorous blebbing of the cell membrane resulting in a motionless carcass of the target cell but not in its total dissolution. Only later this carcass decayed and formed a necrotic ghost. Electron microscopic observations were put into sequence according to microcinematography. Post-recognition phase was characterized by a tight apposition of the membranes of CTL and target cell. No gap junctions could be observed. During target cell disintegration, profound cytoplasmic and nuclear changes occurred simultaneous with surface blebbing. Most noticeable were extensive internal vacuolization, mitochondrial swelling, nuclear pycnosis and dissolution of the nucleolus. These observations suggested that target cell lysis does not start with a surface phenomenon similar to complement lysis, but a process involving practically the whole cell simultaneously. It is conceivable, therefore, that the signal from the CTL is transmitted across the target cell, and that the switch to sudden cell death is manipulated deep inside the cell.

摘要

开展了一项研究,以确定在显微电影摄影术和电子显微镜下T细胞介导的靶细胞裂解的事件顺序。使用预先免疫的脾细胞和纯化程序在体内和体外产生高效细胞毒性T淋巴细胞(CTL)。此类CTL具有高度特异性。这种特异性与CTL和靶标之间形成的黏附数量密切相关,并且该标准被用于研究杀伤性靶细胞相互作用。显微电影摄影术显示,尽管存在时间差异,但单细胞水平的靶细胞裂解可清晰地分为三个阶段:(a)识别阶段,可见CTL在靶细胞表面随机爬行直至建立牢固接触;(b)识别后阶段,在此期间CTL与靶标之间保持牢固接触,而两个细胞均无明显改变;(c)靶细胞崩解阶段,主要特征是细胞膜剧烈起泡,导致靶细胞成为静止的残骸,但并未完全溶解。只有在这之后,残骸才会腐烂并形成坏死的空壳。根据显微电影摄影术对电子显微镜观察结果进行了排序。识别后阶段的特征是CTL和靶细胞的膜紧密并置。未观察到间隙连接。在靶细胞崩解过程中,细胞质和细胞核发生深刻变化,同时伴有表面起泡。最明显的是广泛的内部空泡化、线粒体肿胀、核固缩和核仁溶解。这些观察结果表明,靶细胞裂解并非始于类似于补体裂解的表面现象,而是一个几乎涉及整个细胞的同时发生的过程。因此,可以想象,来自CTL的信号穿过靶细胞传递,并且细胞内深处操控着向突然细胞死亡的转变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f89b/1457473/efe5a42974b6/immunology00267-0017-a.jpg

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