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溶细胞性淋巴细胞对穿孔素介导杀伤的抗性。小鼠细胞毒性T淋巴细胞和人类自然杀伤细胞不含功能性可溶性同源限制因子或其他特异性可溶性保护因子。

Resistance of cytolytic lymphocytes to perforin-mediated killing. Murine cytotoxic T lymphocytes and human natural killer cells do not contain functional soluble homologous restriction factor or other specific soluble protective factors.

作者信息

Jiang S, Persechini P M, Perussia B, Young J D

机构信息

Laboratory of Cellular Physiology and Immunology, Rockefeller University, New York 10021.

出版信息

J Immunol. 1989 Sep 1;143(5):1453-60.

PMID:2503557
Abstract

CTL and NK cells produce a cytolytic pore-forming protein (perforin, cytolysin) localized in their cytoplasmic granules. These cytotoxic cells are resistant to killing mediated by other lymphocytes and by purified perforin. A membrane factor, known as homologous restriction factor (HRF), has been suggested to confer protection to different cell types against both C- and perforin-mediated lysis. The granules of human large granular lymphocytes have been reported to contain, in addition to perforin, a soluble HRF activity that can be eluted from anion-exchange columns at 115 mM NaCl. Here, we report that a soluble HRF activity is absent in the granules or the cytosol of murine CTL and human NK cells. Our data indicate that the inhibition attributed to HRF could be explained by exogenous EDTA added during granule fractionation. EDTA was shown to bind to Mono Q and to elute at 90 to 120 mM NaCl. A second perforin-inhibitory activity was also eluted from such a column. However, it was present in preparations obtained not only from CTL and NK cells, but also from some perforin-susceptible tumor cell lines, indicating that it has nonrestricted distribution and suggesting that it is probably irrelevant to the perforin-protection mechanism. Our results argue against a role for soluble granule HRF or other soluble factors in mediating resistance of cytotoxic lymphocytes against perforin-mediated lysis.

摘要

细胞毒性T淋巴细胞(CTL)和自然杀伤细胞(NK细胞)产生一种位于其细胞质颗粒中的溶细胞性成孔蛋白(穿孔素,溶细胞素)。这些细胞毒性细胞对其他淋巴细胞和纯化穿孔素介导的杀伤具有抗性。一种被称为同源限制因子(HRF)的膜因子被认为可赋予不同细胞类型对补体和穿孔素介导的细胞溶解的保护作用。据报道,人类大颗粒淋巴细胞的颗粒除了含有穿孔素外,还含有一种可溶性HRF活性,该活性可在115 mM氯化钠浓度下从阴离子交换柱上洗脱下来。在此,我们报告在小鼠CTL和人类NK细胞的颗粒或胞质溶胶中不存在可溶性HRF活性。我们的数据表明,归因于HRF的抑制作用可能是由颗粒分级分离过程中添加的外源性乙二胺四乙酸(EDTA)所解释的。已证明EDTA可与Mono Q结合,并在90至120 mM氯化钠浓度下洗脱。第二种穿孔素抑制活性也从此类柱子上洗脱下来。然而,它不仅存在于从CTL和NK细胞获得的制剂中,也存在于一些对穿孔素敏感的肿瘤细胞系的制剂中,这表明它具有非限制性分布,并提示它可能与穿孔素保护机制无关。我们的结果反对可溶性颗粒HRF或其他可溶性因子在介导细胞毒性淋巴细胞对穿孔素介导的细胞溶解的抗性中发挥作用。

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