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基于双亮氨酸的分选信号在一个与基于酪氨酸的基序结合位点不同且调控方式也不同的位点与AP-1的β链结合。

Dileucine-based sorting signals bind to the beta chain of AP-1 at a site distinct and regulated differently from the tyrosine-based motif-binding site.

作者信息

Rapoport I, Chen Y C, Cupers P, Shoelson S E, Kirchhausen T

机构信息

Department of Cell Biology, Harvard Medical School and The Center for Blood Research.

出版信息

EMBO J. 1998 Apr 15;17(8):2148-55. doi: 10.1093/emboj/17.8.2148.

Abstract

In previous work, we showed that peptides from endocytosed proteins containing the tyrosine YXXphi sorting motif are recognized by the mu 2 subunit of AP-2, the plasma membrane clathrin adaptor protein complex. This interaction is activated by phosphoinositide lipids that are phosphorylated at the D-3 position of the inositol ring, and is also enhanced by the formation of clathrin-AP-2 coats. Here, we describe the detection of a specific interaction between peptides containing a second sorting motif, the dileucine motif, and AP-1, the clathrin adaptor complex responsible for sorting proteins at the trans-Golgi network (TGN). Surprisingly, the site of dileucine binding is the beta1 subunit, not mu 1. A YXXphi-containing peptide from a protein trafficked within the TGN does bind to mu 1, however. Phosphatidylinositol 3,4-diphosphate and 3,4, 5-triphosphate did not activate the interaction between dileucine-containing peptides and AP-1 but instead inhibited it, and clathrin-AP-1 coat formation did not alter the interaction. Thus, there are at least two physically separate binding sites for sorting signals on APs, which are also regulated independently.

摘要

在之前的工作中,我们发现,含有酪氨酸YXXphi分选基序的内吞蛋白来源的肽段可被质膜网格蛋白衔接蛋白复合物AP-2的μ2亚基识别。这种相互作用由在肌醇环D-3位磷酸化的磷酸肌醇脂质激活,网格蛋白-AP-2包被的形成也会增强这种相互作用。在此,我们描述了含有第二个分选基序(双亮氨酸基序)的肽段与AP-1(负责在反式高尔基体网络(TGN)分选蛋白的网格蛋白衔接复合物)之间特异性相互作用的检测。令人惊讶的是,双亮氨酸结合位点是β1亚基,而非μ1亚基。然而,来自在TGN内运输的蛋白的含YXXphi肽段确实与μ1亚基结合。磷脂酰肌醇3,4-二磷酸和3,4,5-三磷酸不会激活含双亮氨酸肽段与AP-1之间的相互作用,反而会抑制这种相互作用,并且网格蛋白-AP-1包被的形成不会改变这种相互作用。因此,AP上至少有两个在物理上相互分离的分选信号结合位点,它们也是独立调节的。

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