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AP-2复合物识别内吞分选信号过程中的调控相互作用。

Regulatory interactions in the recognition of endocytic sorting signals by AP-2 complexes.

作者信息

Rapoport I, Miyazaki M, Boll W, Duckworth B, Cantley L C, Shoelson S, Kirchhausen T

机构信息

Department of Cell Biology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

EMBO J. 1997 May 1;16(9):2240-50. doi: 10.1093/emboj/16.9.2240.

Abstract

Many plasma membrane proteins destined for endocytosis are concentrated into clathrin-coated pits through the recognition of a tyrosine-based motif in their cytosolic domains by an adaptor (AP-2) complex. The mu2 subunit of isolated AP-2 complexes binds specifically, but rather weakly, to proteins bearing the tyrosine-based signal. We now demonstrate, using peptides with a photoreactive probe, that this binding is strengthened significantly when the AP-2 complex is present in clathrin coats, indicating that there is cooperativity between receptor-AP-2 interactions and coat formation. Phosphoinositides with a phosphate at the D-3 position of the inositol ring, but not other isomers, also increase the affinity of the AP-2 complex for the tyrosine-based motif. AP-2 is the first protein known (in any context) to interact with phosphatidylinositol 3-phosphate. Our findings indicate that receptor recruitment can be coupled to clathrin coat assembly and suggest a mechanism for regulation of membrane traffic by lipid products of phosphoinositide 3-kinases.

摘要

许多注定要进行内吞作用的质膜蛋白通过衔接蛋白(AP-2)复合物识别其胞质结构域中基于酪氨酸的基序,从而聚集到网格蛋白包被小窝中。分离出的AP-2复合物的μ2亚基与带有基于酪氨酸信号的蛋白特异性结合,但结合较弱。我们现在使用带有光反应性探针的肽证明,当AP-2复合物存在于网格蛋白包被中时,这种结合会显著增强,这表明受体与AP-2的相互作用和包被形成之间存在协同作用。肌醇环D-3位带有磷酸的磷酸肌醇,而非其他异构体,也会增加AP-2复合物对基于酪氨酸基序的亲和力。AP-2是已知的(在任何情况下)首个与磷脂酰肌醇3-磷酸相互作用的蛋白。我们的研究结果表明,受体募集可以与网格蛋白包被组装相偶联,并提示了一种由磷酸肌醇3-激酶的脂质产物调节膜运输的机制。

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