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信号转导分子和糖基磷脂酰肌醇连接蛋白在MDCK细胞中形成富含小窝蛋白的不溶性复合物。

Signal transducing molecules and glycosyl-phosphatidylinositol-linked proteins form a caveolin-rich insoluble complex in MDCK cells.

作者信息

Sargiacomo M, Sudol M, Tang Z, Lisanti M P

机构信息

Whitehead Institute for Biomedical Research, Cambridge, Massachusetts 02142-1479.

出版信息

J Cell Biol. 1993 Aug;122(4):789-807. doi: 10.1083/jcb.122.4.789.

Abstract

GPI-linked protein molecules become Triton-insoluble during polarized sorting to the apical cell surface of epithelial cells. These insoluble complexes, enriched in cholesterol, glycolipids, and GPI-linked proteins, have been isolated by flotation on sucrose density gradients and are thought to contain the putative GPI-sorting machinery. As the cellular origin and molecular protein components of this complex remain unknown, we have begun to characterize these low-density insoluble complexes isolated from MDCK cells. We find that these complexes, which represent 0.4-0.8% of the plasma membrane, ultrastructurally resemble caveolae and are over 150-fold enriched in a model GPI-anchored protein and caveolin, a caveolar marker protein. However, they exclude many other plasma membrane associated molecules and organelle-specific marker enzymes, suggesting that they represent microdomains of the plasma membrane. In addition to caveolin, these insoluble complexes contain a subset of hydrophobic plasma membrane proteins and cytoplasmically-oriented signaling molecules, including: (a) GTP-binding proteins--both small and heterotrimeric; (b) annex II--an apical calcium-regulated phospholipid binding protein with a demonstrated role in exocytic fusion events; (c) c-Yes--an apically localized member of the Src family of non-receptor type protein-tyrosine kinases; and (d) an unidentified serine-kinase activity. As we demonstrate that caveolin is both a transmembrane molecule and a major phospho-acceptor component of these complexes, we propose that caveolin could function as a transmembrane adaptor molecule that couples luminal GPI-linked proteins with cytoplasmically oriented signaling molecules during GPI-membrane trafficking or GPI-mediated signal transduction events. In addition, our results have implications for understanding v-Src transformation and the actions of cholera and pertussis toxins on hetero-trimeric G proteins.

摘要

糖基磷脂酰肌醇(GPI)连接的蛋白质分子在上皮细胞向顶端细胞表面进行极化分选的过程中会变得不溶于Triton。这些富含胆固醇、糖脂和GPI连接蛋白的不溶性复合物,已通过在蔗糖密度梯度上漂浮分离出来,并且被认为包含假定的GPI分选机制。由于这种复合物的细胞起源和分子蛋白成分仍然未知,我们已开始对从MDCK细胞中分离出的这些低密度不溶性复合物进行表征。我们发现这些复合物占质膜的0.4 - 0.8%,在超微结构上类似于小窝,并且在一种模型GPI锚定蛋白和小窝标记蛋白小窝蛋白中富集超过150倍。然而,它们排除了许多其他质膜相关分子和细胞器特异性标记酶,这表明它们代表质膜的微区。除了小窝蛋白外,这些不溶性复合物还包含一部分疏水质膜蛋白和面向细胞质的信号分子,包括:(a)GTP结合蛋白——小的和异源三聚体的;(b)膜联蛋白II——一种顶端钙调节的磷脂结合蛋白,已证明在胞吐融合事件中起作用;(c)c-Yes——非受体型蛋白酪氨酸激酶Src家族的顶端定位成员;以及(d)一种未鉴定的丝氨酸激酶活性。由于我们证明小窝蛋白既是一种跨膜分子,也是这些复合物的主要磷酸化受体成分,我们提出小窝蛋白可以作为一种跨膜衔接分子,在GPI膜运输或GPI介导的信号转导事件中,将腔内GPI连接蛋白与面向细胞质的信号分子偶联起来。此外,我们的结果对于理解v-Src转化以及霍乱毒素和百日咳毒素对异源三聚体G蛋白的作用具有启示意义。

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