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Bazooka-Stardust 复合物的形成对于上皮细胞的质膜极性至关重要。

Formation of a Bazooka-Stardust complex is essential for plasma membrane polarity in epithelia.

机构信息

Abteilung Stammzellbiologie, Forschungszentrum der Deutschen Forschungsgemeinschaft für Molekularphysiologie des Gehirns (CMPB), Georg-August-Universität Göttingen, 37077 Göttingen, Germany.

出版信息

J Cell Biol. 2010 Sep 6;190(5):751-60. doi: 10.1083/jcb.201006029.

Abstract

Apical-basal polarity in Drosophila melanogaster epithelia depends on several evolutionarily conserved proteins that have been assigned to two distinct protein complexes: the Bazooka (Baz)-PAR-6 (partitioning defective 6)-atypical protein kinase C (aPKC) complex and the Crumbs (Crb)-Stardust (Sdt) complex. These proteins operate in a functional hierarchy, in which Baz is required for the proper subcellular localization of all other proteins. We investigated how these proteins interact and how this interaction is regulated. We show that Baz recruits Sdt to the plasma membrane by direct interaction between the Postsynaptic density 95/Discs large/Zonula occludens 1 (PDZ) domain of Sdt and a region of Baz that contains a phosphorylation site for aPKC. Phosphorylation of Baz causes the dissociation of the Baz-Sdt complex. Overexpression of a nonphosphorylatable version of Baz blocks the dissociation of Sdt from Baz, causing phenotypes very similar to those of crb and sdt mutations. Our findings provide a molecular mechanism for the phosphorylation-dependent interaction between the Baz-PAR-3 and Crb complexes during the establishment of epithelial polarity.

摘要

果蝇表皮的顶端-基底极性依赖于几种进化上保守的蛋白质,这些蛋白质被分配到两个不同的蛋白质复合物中:Bazooka(Baz)-PAR-6(partitioning defective 6)-非典型蛋白激酶 C(aPKC)复合物和 Crumbs(Crb)-Stardust(Sdt)复合物。这些蛋白质在功能上具有层次结构,其中 Baz 对于所有其他蛋白质的正确亚细胞定位是必需的。我们研究了这些蛋白质如何相互作用以及这种相互作用如何受到调节。我们表明,Baz 通过 Sdt 的 Postsynaptic density 95/Discs large/Zonula occludens 1(PDZ)结构域与 Baz 中包含 aPKC 磷酸化位点的区域之间的直接相互作用将 Sdt 募集到质膜。Baz 的磷酸化导致 Baz-Sdt 复合物的解离。过量表达一种不可磷酸化的 Baz 版本会阻止 Sdt 从 Baz 解离,导致与 crb 和 sdt 突变非常相似的表型。我们的发现为 Baz-PAR-3 和 Crb 复合物在建立上皮极性过程中磷酸化依赖性相互作用提供了一个分子机制。

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