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T细胞介导的细胞毒性机制。VIII. 吞噬残质对应于导致细胞裂解步骤中的不可逆阶段(裂解编程)。

The mechanism of T-cell mediated cytotoxicity. VIII. Zeiosis corresponds to irreversible phase (programming for lysis) in steps leading to lysis.

作者信息

Sanderson C J

出版信息

Immunology. 1981 Feb;42(2):201-6.

Abstract

The combined use of an improved technique for inactivating cytotoxic T cells during the lytic reaction, with time lapse cinematography and isotope release assay, have shown that the initiation of the morphological phase of zeiosis corresponds to the time when the target cell is irreversibly programmed to lyse. It is suggested that rubidium release occurs during the phase of zeiosis. The rate of release of chromium is the result of two phases of variable length, The reversible phase (before programming for lysis) and the irreversible phase from the initiation of zeiosis to the final lytic event. The time required for programming for lysis to occur depends on the number of T cells reacting with the target cell. Thus at high ratios in tubes, where multiple interactions are possible, most target cells are programmed to lyse within 10 min. However, under conditions when T-cell:target-cell conjugates are kept in suspension to prevent multiple interactions, programming for lysis can take several hours. This provides an explanation for the apparent difference in timing of zeiosis and programming for lysis in previous publications. It is also shown that further T-cell interactions with the target cell after programming for lysis (i.e. during the irreversible phase), markedly influence the rate of chromium release. This provides an explanation for the fact that chromium release takes at least 3 h to reach plateau levels after inactivation of the T cells, whereas at high effector cell ratios, maximum levels of chromium release can occur within 1 h.

摘要

在溶解反应期间,将一种改进的用于使细胞毒性T细胞失活的技术与延时摄影术和同位素释放测定相结合,结果表明,胞质皱缩的形态学阶段的起始与靶细胞被不可逆地编程为裂解的时间相对应。有人提出,铷的释放在胞质皱缩阶段发生。铬的释放速率是两个长度可变阶段的结果,即可逆阶段(在编程裂解之前)和从胞质皱缩起始到最终裂解事件的不可逆阶段。编程裂解发生所需的时间取决于与靶细胞反应的T细胞数量。因此,在试管中比例较高时,由于可能发生多次相互作用,大多数靶细胞在10分钟内被编程为裂解。然而,在T细胞与靶细胞共轭物保持悬浮以防止多次相互作用的条件下,编程裂解可能需要数小时。这为先前出版物中胞质皱缩和编程裂解时间上的明显差异提供了解释。还表明,在编程裂解后(即在不可逆阶段)T细胞与靶细胞的进一步相互作用,显著影响铬的释放速率。这为以下事实提供了解释:在T细胞失活后,铬的释放至少需要3小时才能达到平台水平,而在高效应细胞比例下,铬释放的最大水平可在1小时内出现。

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