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Fc受体介导的吞噬作用中信号传导的协调。

The coordination of signaling during Fc receptor-mediated phagocytosis.

作者信息

Swanson Joel A, Hoppe Adam D

机构信息

University of Michigan Medical School, 1335 Catherine Street, Med Sci II, Rm. 5608, Ann Arbor, MI 48109-0620, USA.

出版信息

J Leukoc Biol. 2004 Dec;76(6):1093-103. doi: 10.1189/jlb.0804439. Epub 2004 Oct 5.

Abstract

Phagocytosis by macrophages can be initiated by Fcgamma receptors (FcR) in membranes that bind to Fc regions of immunoglobulin G (IgG). Activated FcR transduce signals to cytoplasm, which regulate the internalization of IgG-coated particles into plasma membrane-derived vacuoles, phagosomes. Particles internalized by phagocytosis are much larger than FcR, which prompts questions of if and how the receptors are coordinated with each other. FcR-mediated signal transduction entails recruitment of proteins from cytoplasm to the receptor, largely via protein phosphorylation. These FcR signaling complexes then activate proteins that regulate actin, myosin, membrane fusion, and the production of reactive oxygen intermediates. Recent fluorescence microscopic studies of phagocytosis in macrophages indicate that signaling by FcR occurs as a sequence of distinct stages, evident in the spatial and temporal patterns of phosphoinositides, protein kinase C, and Rho-family GTPase activation on forming phagosomes. The coordination of these stages may be regulated by lipids or lipid-anchored proteins, which diffuse away from FcR complexes. Lateral diffusion of FcR-derived signals could integrate FcR-dependent responses over large areas of membrane in the forming phagosome.

摘要

巨噬细胞的吞噬作用可由细胞膜上的Fcγ受体(FcR)启动,该受体与免疫球蛋白G(IgG)的Fc区域结合。活化的FcR将信号传导至细胞质,调节包被IgG的颗粒内化到源自质膜的液泡即吞噬体中。通过吞噬作用内化的颗粒比FcR大得多,这引发了关于受体是否以及如何相互协调的问题。FcR介导的信号转导需要将细胞质中的蛋白质募集到受体上,主要通过蛋白质磷酸化实现。这些FcR信号复合物随后激活调节肌动蛋白、肌球蛋白、膜融合和活性氧中间体产生的蛋白质。最近对巨噬细胞吞噬作用的荧光显微镜研究表明,FcR信号传导以一系列不同阶段发生,这在吞噬体形成过程中磷酸肌醇、蛋白激酶C和Rho家族GTP酶激活的空间和时间模式中很明显。这些阶段的协调可能受脂质或脂质锚定蛋白调节,它们从FcR复合物扩散开来。FcR衍生信号的侧向扩散可整合形成中的吞噬体大片膜区域上的FcR依赖性反应。

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