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首页> 外文期刊>Molecular biology of the cell >MARK2/EMMK1/Par-1B alpha phosphorylation of Rab11-family interacting protein 2 is necessary for the timely establishment of polarity in Madin-Darby canine kidney cells
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MARK2/EMMK1/Par-1B alpha phosphorylation of Rab11-family interacting protein 2 is necessary for the timely establishment of polarity in Madin-Darby canine kidney cells

机译:Rab11家庭相互作用蛋白2的MARK2 / EMMK1 / Par-1Bα磷酸化对于及时建立Madin-Darby犬肾细胞的极性是必要的

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摘要

Rab11a, myosin Vb, and the Rab11-family interacting protein 2 (FIP2) regulate plasma membrane recycling in epithelial cells. This study sought to characterize more fully Rab11-FIP2 function by identifying kinase activities modifying Rab11-FIP2. We have found that gastric microsomal membrane extracts phosphorylate Rab11-FIP2 on serine 227. We identified the kinase that phosphorylated Rab11-FIP2 as MARK2/EMK1/Par-1B alpha (MARK2), and recombinant MARK2 phosphorylated Rab11-FIP2 only on serine 227. We created stable Madin-Darby canine kidney (MDCK) cell lines expressing enhanced green fluorescent protein-Rab11-FIP2 wild type or a nonphosphorylatable mutant [Rab11-FIP2(S227A)]. Analysis of these cell lines demonstrates a new role for Rab11-FIP2 in addition to that in the plasma membrane recycling system. In calcium switch assays, cells expressing Rab11-FIP2(S227A) showed a defect in the timely reestablishment of p120-containing junctional complexes. However, Rab11-FIP2(S227A) did not affect localization with recycling system components or the normal function of apical recycling and transcytosis pathways. These results indicate that phosphorylation of Rab11-FIP2 on serine 227 by MARK2 regulates an alternative pathway modulating the establishment of epithelial polarity.
机译:Rab11a,肌球蛋白Vb和Rab11家族相互作用蛋白2(FIP2)调节上皮细胞中的质膜回收。这项研究试图通过鉴定修饰Rab11-FIP2的激酶活性来更全面地表征Rab11-FIP2的功能。我们发现胃微粒体膜提取物在丝氨酸227上磷酸化Rab11-FIP2。我们鉴定了磷酸化Rab11-FIP2的激酶为MARK2 / EMK1 / Par-1Bα(MARK2),而重组MARK2仅在丝氨酸227上磷酸化了Rab11-FIP2。我们创建了稳定的Madin-Darby犬肾(MDCK)细胞系,该细胞系表达增强的绿色荧光蛋白-Rab11-FIP2野生型或不可磷酸化突变体[Rab11-FIP2(S227A)]。对这些细胞系的分析表明,除了在质膜回收系统中,Rab11-FIP2还具有新的作用。在钙转换试验中,表达Rab11-FIP2(S227A)的细胞在及时重建含p120的连接复合体中显示出缺陷。但是,Rab11-FIP2(S227A)不会影响回收系统组件的定位或根尖回收和转胞吞途径的正常功能。这些结果表明MARK2丝氨酸227上的Rab11-FIP2的磷酸化调节了调节上皮极性建立的替代途径。

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