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A Highlights from MBoC Selection: Overlapping Roles of Drosophila Drak and Rok Kinases in Epithelial Tissue Morphogenesis

机译:MBoC选择的亮点:果蝇Drak和Rok激酶在上皮组织形态发生中的重叠作用

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Dynamic regulation of cytoskeletal contractility through phosphorylation of the nonmuscle Myosin-II regulatory light chain (MRLC) provides an essential source of tension for shaping epithelial tissues. Rho GTPase and its effector kinase ROCK have been implicated in regulating MRLC phosphorylation in vivo, but evidence suggests that other mechanisms must be involved. Here, we report the identification of a single Drosophila homologue of the Death-associated protein kinase (DAPK) family, called Drak, as a regulator of MRLC phosphorylation. Based on analysis of null mutants, we find that Drak broadly promotes proper morphogenesis of epithelial tissues during development. Drak activity is largely redundant with that of the Drosophila ROCK orthologue, Rok, such that it is essential only when Rok levels are reduced. We demonstrate that these two kinases synergistically promote phosphorylation of Spaghetti squash (Sqh), the Drosophila MRLC orthologue, in vivo. The lethality of drak/rok mutants can be rescued by restoring Sqh activity, indicating that Sqh is the critical common effector of these two kinases. These results provide the first evidence that DAPK family kinases regulate actin dynamics in vivo and identify Drak as a novel component of the signaling networks that shape epithelial tissues.
机译:通过非肌肉肌球蛋白II调节轻链(MRLC)磷酸化来动态调节细胞骨架的收缩力,为上皮组织的形成提供了重要的张力来源。 Rho GTPase及其效应激酶ROCK与体内调节MRLC磷酸化有关,但证据表明必须涉及其他机制。在这里,我们报告的死亡相关蛋白激酶(DAPK)家族,称为Drak,作为MRLC磷酸化的调节剂的单个果蝇同源物的鉴定。基于无效突变体的分析,我们发现Drak在发育过程中广泛促进上皮组织的适当形态发生。 Drak活性与果蝇ROCK直系同源基因Rok在很大程度上是多余的,因此仅当Rok含量降低时才有必要。我们证明这两种激酶在体内协同促进意大利面条南瓜(Sqh),果蝇MRLC直系同源物的磷酸化。可以通过恢复Sqh活性来挽救drak / rok突变体的致死性,这表明Sqh是这两种激酶的关键共同效应物。这些结果提供了第一个证据,证明DAPK家族激酶在体内调节肌动蛋白的动力学,并将Drak鉴定为塑造上皮组织的信号网络的新组成部分。

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