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内吞作用、膜循环与Fc受体功能。

Endocytosis, membrane recycling and Fc receptor function.

作者信息

Mellman I S

出版信息

Ciba Found Symp. 1982(92):35-58.

PMID:6924894
Abstract

We have studied the composition and fate of plasma membrane internalized during both fluid-phase and receptor-mediated endocytosis in mouse macrophages. Particular attention has been paid to the macrophage Fc receptor, an intrinsic membrane glycoprotein that we have isolated and characterized biochemically and immunologically. Monoclonal and polyclonal antibodies directed against the receptor and against a series of other unrelated plasma membrane proteins have been used. In addition, we have used radioiodination techniques to label selectively the polypeptides of pinocytic vesicle membrane from within intact cells. Our results indicate that fluid pinocytosis in macrophages involves the internalization of a largely representative sample of plasma membrane polypeptides. Significantly, the Fc receptor seems to be internalized at a rate similar to that of most other membrane proteins. However, selective internalization of the receptor is induced during the endocytosis of certain ligands. The phagocytosis of immunoglobulin G (IgG)-coated erythrocyte ghosts results in the selective and largely irreversible removal of Fc receptors from the macrophage surface. Selectively internalized receptors do not recycle but are rapidly degraded. Fc receptors also appear to be preferentially interiorized during the rapid pinocytosis of IgG-containing soluble immune complexes. Uptake is accompanied by a sharp decrease in the number of surface receptors, which is partially reversed after the removal of ligand.

摘要

我们研究了小鼠巨噬细胞在液相内吞作用和受体介导的内吞作用过程中内化的质膜的组成和命运。我们特别关注巨噬细胞Fc受体,这是一种内在膜糖蛋白,我们已经对其进行了生化和免疫学分离及表征。已使用针对该受体以及一系列其他不相关质膜蛋白的单克隆抗体和多克隆抗体。此外,我们使用放射性碘化技术从完整细胞内部选择性标记胞饮小泡膜的多肽。我们的结果表明,巨噬细胞中的液相胞饮作用涉及质膜多肽的一个具有很大代表性的样本的内化。值得注意的是,Fc受体似乎以内化速率与大多数其他膜蛋白相似。然而,在某些配体的内吞作用过程中会诱导受体的选择性内化。免疫球蛋白G(IgG)包被的红细胞幽灵的吞噬作用导致Fc受体从巨噬细胞表面选择性且在很大程度上不可逆地去除。选择性内化的受体不会再循环而是迅速降解。在含IgG的可溶性免疫复合物的快速胞饮作用过程中,Fc受体似乎也优先内化。摄取伴随着表面受体数量的急剧减少,在去除配体后部分逆转。

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