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在表皮生长因子受体的加工过程中,膜联蛋白I在多囊泡小体中被磷酸化。

Annexin I is phosphorylated in the multivesicular body during the processing of the epidermal growth factor receptor.

作者信息

Futter C E, Felder S, Schlessinger J, Ullrich A, Hopkins C R

机构信息

MRC Laboratory for Molecular Cell Biology, University College, London.

出版信息

J Cell Biol. 1993 Jan;120(1):77-83. doi: 10.1083/jcb.120.1.77.

Abstract

We have previously shown that an active epidermal growth factor receptor (EGF-R) kinase is necessary for efficient sorting of the EGF-R to the lysosome, and we have shown that this occurs in the multivesicular body (MVB), where EGF-R are sorted away from recycling receptors by being removed to the internal vesicles of the MVB. The aim of the present study was to identify substrates of the EGF-R kinase associated with MVBs which might play a role in this sorting process. We used a density shift technique to isolate MVBs and show that the major substrates phosphorylated in vitro within MVBs which contain an active EGF-R kinase are the EGF-R itself and annexin I. Annexin I is associated with both plasma membrane and MVBs in a calcium-independent manner but can be phosphorylated in vitro only in MVBs. Phosphorylation of calcium-independent annexin I in isolated MVBs converts it to a form that requires calcium for membrane association. In cells with an active EGF-R kinase the amount of calcium-independent annexin I in MVBs is reduced, suggesting that a phosphorylation-induced conversion of the calcium independent to the calcium-dependent form also occurs in vivo. Our observations, together with the known properties of annexin I in mediating membrane fusion, suggest that inward vesiculation in MVBs is induced by the EGF-R and is mediated by phosphorylated annexin I.

摘要

我们之前已经表明,活性表皮生长因子受体(EGF-R)激酶对于将EGF-R有效分选至溶酶体是必需的,并且我们已经表明这发生在多囊泡体(MVB)中,在那里EGF-R通过被转运至MVB的内部囊泡而与循环受体分离。本研究的目的是鉴定与MVB相关的EGF-R激酶的底物,这些底物可能在该分选过程中发挥作用。我们使用密度转移技术分离MVB,并表明在含有活性EGF-R激酶的MVB中体外磷酸化的主要底物是EGF-R本身和膜联蛋白I。膜联蛋白I以钙非依赖性方式与质膜和MVB相关联,但仅在MVB中可在体外被磷酸化。在分离的MVB中钙非依赖性膜联蛋白I的磷酸化将其转化为一种需要钙才能与膜结合的形式。在具有活性EGF-R激酶的细胞中,MVB中钙非依赖性膜联蛋白I的量减少,这表明在体内也发生了磷酸化诱导的钙非依赖性形式向钙依赖性形式的转化。我们的观察结果,连同膜联蛋白I在介导膜融合方面的已知特性,表明MVB中的内向囊泡形成是由EGF-R诱导的,并由磷酸化的膜联蛋白I介导。

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