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人T淋巴细胞中白细胞介素2受体的内吞作用:受体α、β和γ链在细胞内的不同定位及命运

Endocytosis of interleukin 2 receptors in human T lymphocytes: distinct intracellular localization and fate of the receptor alpha, beta, and gamma chains.

作者信息

Hémar A, Subtil A, Lieb M, Morelon E, Hellio R, Dautry-Varsat A

机构信息

Unité de Biologie des Interactions Cellulaires, URA CNRS 1960, Institut Pasteur, Paris, France.

出版信息

J Cell Biol. 1995 Apr;129(1):55-64. doi: 10.1083/jcb.129.1.55.

Abstract

Members of the cytokine receptor family are composed of several noncovalently linked chains with sequence and structure homologies in their extracellular domain. Receptor subfamily members share at least one component: thus the receptors for interleukin (IL) 2 and IL15 have common beta and gamma chains, while those for IL2, 4, 7, and 9 have a common gamma chain. The intracellular pathway followed by IL2 receptors after ligand binding and endocytosis was analyzed by immunofluorescence and confocal microscopy in a human T lymphocytic cell line. Surprisingly, the alpha, beta, and gamma chains had different intracellular localizations after being endocytosed together. The alpha chain was always in transferrin-positive compartments (early/recycling endosomes), both at early and late internalization times, but was never detected in rab7-positive compartments (late endosomes). On the other hand, at late internalization times, the beta and gamma chains were excluded from transferrin-positive organelles and did not colocalize with alpha. Furthermore, beta could be found in rab7-positive vesicles. These differences suggest that the alpha chain recycles to the plasma membrane, while the beta and gamma chains are sorted towards the degradation pathway. The half-lives of these three chains on the cell surface also reflect their different intracellular fates after endocytosis. The beta and gamma chains are very short-lived polypeptides since their half-life on the surface is only approximately 1 h, whereas alpha is a much more stable surface protein. This shows for the first time that components of a multimeric receptor can be sorted separately along the endocytic pathway.

摘要

细胞因子受体家族成员由几条在细胞外结构域具有序列和结构同源性的非共价连接链组成。受体亚家族成员至少共享一个组分:因此,白细胞介素(IL)2和IL15的受体具有共同的β链和γ链,而IL2、4、7和9的受体具有共同的γ链。通过免疫荧光和共聚焦显微镜在人T淋巴细胞系中分析了IL2受体在配体结合和内吞作用后所遵循的细胞内途径。令人惊讶的是,α链、β链和γ链在内吞后一起具有不同的细胞内定位。α链在早期和晚期内化时始终处于转铁蛋白阳性区室(早期/再循环内体)中,但从未在rab7阳性区室(晚期内体)中检测到。另一方面,在晚期内化时,β链和γ链被排除在转铁蛋白阳性细胞器之外,并且不与α链共定位。此外,β链可在rab7阳性囊泡中发现。这些差异表明α链循环回到质膜,而β链和γ链则被分选到降解途径。这三条链在细胞表面的半衰期也反映了它们在内吞作用后不同的细胞内命运。β链和γ链是非常短命的多肽,因为它们在表面的半衰期仅约1小时,而α链是一种更稳定的表面蛋白。这首次表明多聚体受体的组分可以沿着内吞途径被分别分选。

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