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有证据表明人类白细胞的超氧化物生成系统与细胞表面相关。

Evidence that the superoxide-generating system of human leukocytes is associated with the cell surface.

作者信息

Goldstein I M, Cerqueira M, Lind S, Kaplan H B

出版信息

J Clin Invest. 1977 Feb;59(2):249-54. doi: 10.1172/JCI108635.

Abstract

Superoxide anion (O-2-) generation by human peripheral blood polymorphonuclear leukocytes is enhanced when these cells encounter appropriate soluble or particulate stimuli. O-2- generation requires intact, viable cells and proceeds independently of phagocytosis. To investigate the possibility that the O-2--generating system is associated with the outer surface of the polymorphonuclear leukocyte plasma membrane, we have examined the effects upon O-2- production of p-diazobenzenesulfonic acid, a reagent which can react predominantly with proteins of the external cell membrane. When normal human polymorphonuclear leukocytes were preincubated with cytochalasin B (to minimize endocytosis) and then exposed to the surface-active lectin, concanavalin A, the cells were stimulated to generate O-2- in a concentration- and time-dependent fashion and selectively to discharge the granule-associated enzyme, lysozyme, into the surrounding medium. These responses, as well as cellular binding of [H] concanavalin A, could be blocked by alpha-methyl-D-mannoside. Brief treatment (less than 5 min at 4 degrees C) of the cells with p-diazobenzenesulfonic acid (1.0-5.0 mM) significantly interfered with concanavalin A-mediated O-2- generation but had no influence upon lysozyme release or upon binding of [3H] concanavalin A. The diazonium salt did not alter cell viability or the specific activity of the cytoplasmic enzyme, lactate dehydrogenase (inhibitable under conditions which allowed entry of this reagent into the cytosol). p-Diazobenzenesulfonic acid, therefore, very likely exerted its effects at the cell surface of the intact polymorphonuclear leukocyte, selectively inhibiting O-2- production (either directly or indirectly) without influencing another response to lectin-cell contact: release of lysozyme. These results support the possibility that a polymorphonuclear leukocyte ectoenzyme is responsible for O-2- production.

摘要

当人类外周血多形核白细胞遇到合适的可溶性或颗粒性刺激物时,其超氧阴离子(O₂⁻)的生成会增强。O₂⁻的生成需要完整、有活力的细胞,且独立于吞噬作用进行。为了研究O₂⁻生成系统是否与多形核白细胞质膜的外表面相关,我们检测了对氨基苯磺酸对O₂⁻生成的影响,该试剂主要与细胞膜外部的蛋白质发生反应。当正常人多形核白细胞先用细胞松弛素B预孵育(以尽量减少内吞作用),然后暴露于表面活性凝集素伴刀豆球蛋白A时,细胞被刺激以浓度和时间依赖性方式生成O₂⁻,并选择性地将颗粒相关酶溶菌酶释放到周围介质中。这些反应以及[³H]伴刀豆球蛋白A的细胞结合可被α-甲基-D-甘露糖苷阻断。用对氨基苯磺酸(1.0 - 5.0 mM)对细胞进行短暂处理(4℃下少于5分钟)会显著干扰伴刀豆球蛋白A介导的O₂⁻生成,但对溶菌酶释放或[³H]伴刀豆球蛋白A的结合没有影响。重氮盐不会改变细胞活力或细胞质酶乳酸脱氢酶的比活性(在允许该试剂进入细胞质溶胶的条件下可被抑制)。因此,对氨基苯磺酸很可能在完整的多形核白细胞的细胞表面发挥作用,选择性抑制O₂⁻生成(直接或间接),而不影响对凝集素 - 细胞接触的另一种反应:溶菌酶的释放。这些结果支持了多形核白细胞外切酶负责O₂⁻生成的可能性。

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