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中性粒细胞的功能反应取决于免疫复合物的价态。

Neutrophil functional responses depend on immune complex valency.

作者信息

Strohmeier G R, Brunkhorst B A, Seetoo K F, Bernardo J, Weil G J, Simons E R

机构信息

Department of Biochemistry, Boston University School of Medicine, Massachusetts 02118, USA.

出版信息

J Leukoc Biol. 1995 Oct;58(4):403-14. doi: 10.1002/jlb.58.4.403.

Abstract

Ligand-induced cross-linking of Fc gamma receptors (Fc gamma R) on neutrophils plays a significant role in their stimulation, shown here by contrasting the responses induced by low valency immune complexes (LICs) and high valency immune complexes (HICs) and by cross-linking LICs in situ (L/Ab) after their addition to the cells. Multiparameter flow cytometry was used to measure immune complex (IC)-elicited changes in cytoplasmic Ca2+ concentration and initiation of the oxidative burst simultaneously in the same cell and to correlate these with Fc gamma R occupancy. We have previously shown that subpopulations of neutrophils respond maximally to subsaturating concentrations of HIC; saturating dosages stimulate the entire population. This discrepancy was not due to differences in receptor occupancy. The magnitude of the transient Ca2+ increase was independent of the dose of HIC but depended on the dose when an LIC was used. As shown here, L/Ab cross-linking elicited Ca2+ responses similar to those observed in HIC-stimulated cells. In contrast, LIC elicited only minimal intracellular delta pH and no oxidative burst or membrane potential changes at all unless Fc gamma R was cross-linked, accomplished by HIC or by L/Ab. However, azurophilic degranulation, as determined by elastase release, was not observed in cells stimulated by the in situ cross-linking method, whereas the HIC preparation triggered azurophilic degranulation. Thus, some Fc gamma R-mediated neutrophil effector functions such as azurophilic degranulation and oxidative burst initiation have an absolute requirement for Fc gamma R cross-linking, whereas signaling functions such as changes in membrane potential, intracellular pH, and intracellular Ca2+ concentration can occur, albeit more slowly and to a lesser extent, if single Fc gamma R are occupied.

摘要

配体诱导中性粒细胞上的Fcγ受体(FcγR)交联在其激活过程中发挥重要作用,这一点通过对比低价免疫复合物(LICs)和高价免疫复合物(HICs)诱导的反应以及在LICs添加到细胞后原位交联LICs(L/Ab)得以体现。多参数流式细胞术用于在同一细胞中同时测量免疫复合物(IC)引发的细胞质Ca2+浓度变化和氧化爆发的启动,并将这些与FcγR占有率相关联。我们之前已经表明,中性粒细胞亚群对低于饱和浓度的HIC反应最大;饱和剂量刺激整个群体。这种差异并非由于受体占有率的不同。Ca2+瞬时增加的幅度与HIC剂量无关,但使用LIC时则取决于剂量。如此处所示,L/Ab交联引发的Ca2+反应与HIC刺激细胞中观察到的反应相似。相比之下,LIC仅引发最小的细胞内ΔpH变化,并且根本不会引发氧化爆发或膜电位变化,除非FcγR被交联,这可通过HIC或L/Ab实现。然而,通过弹性蛋白酶释放测定,原位交联方法刺激的细胞中未观察到嗜天青颗粒脱粒,而HIC制剂引发了嗜天青颗粒脱粒。因此,一些FcγR介导的中性粒细胞效应功能,如嗜天青颗粒脱粒和氧化爆发启动,绝对需要FcγR交联,而信号功能,如膜电位、细胞内pH和细胞内Ca2+浓度的变化,即使单个FcγR被占据,也可能发生,尽管速度较慢且程度较小。

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