首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Anoctamin 1 (Tmem16A) Ca2+-activated chloride channel stoichiometrically interacts with an ezrin–radixin–moesin network
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Anoctamin 1 (Tmem16A) Ca2+-activated chloride channel stoichiometrically interacts with an ezrin–radixin–moesin network

机译:蛋氨酸1(Tmem16A)Ca2 +激活的氯离子通道与ezrin-radixin-moesin网络化学计量相互作用

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摘要

The newly discovered Ca2+-activated Cl channel (CaCC), Anoctamin 1 (Ano1 or TMEM16A), has been implicated in vital physiological functions including epithelial fluid secretion, gut motility, and smooth muscle tone. Overexpression of Ano1 in HEK cells or Xenopus oocytes is sufficient to generate Ca2+-activated Cl currents, but the details of channel composition and the regulatory factors that control channel biology are incompletely understood. We used a highly sensitive quantitative SILAC proteomics approach to obtain insights into stoichiometric protein networks associated with the Ano1 channel. These studies provide a comprehensive footprint of putative Ano1 regulatory networks. We find that Ano1 associates with the signaling/scaffolding proteins ezrin, radixin, moesin, and RhoA, which link the plasma membrane to the cytoskeleton with very high stoichiometry. Ano1, ezrin, and moesin/radixin colocalize apically in salivary gland epithelial cells, and overexpression of moesin and Ano1 in HEK cells alters the subcellular localization of both proteins. Moreover, interfering RNA for moesin modifies Ano1 current without affecting its surface expression level. Another network associated with Ano1 includes the SNARE and SM proteins VAMP3, syntaxins 2 and -4, and syntaxin-binding proteins munc18b and munc18c, which are integral to translocation of vesicles to the plasma membrane. A number of other regulatory proteins, including GTPases, Ca2+-binding proteins, kinases, and lipid-interacting proteins are enriched in the Ano1 complex. These data provide stoichiometrically prioritized information about mechanisms regulating Ano1 function and trafficking to polarized domains of the plasma membrane.
机译:新发现的Ca 2 + 激活的Cl -通道(CaCC)的Anoctamin 1(Ano1或TMEM16A)与重要的生理功能有关,包括上皮液分泌,肠道运动力和平滑肌音。 HEK细胞或爪蟾卵母细胞中Ano1的过表达足以产生Ca 2 + 激活的Cl -电流,但是通道组成的细节和控制通道生物学的调节因子尚未完全了解。我们使用了高度灵敏的定量SILAC蛋白质组学方法,以了解与Ano1通道相关的化学计量蛋白质网络。这些研究提供了假定的Ano1监管网络的全面足迹。我们发现,Ano1与信号/支架蛋白ezrin,辐射素,肌球蛋白和RhoA相关联,后者以非常高的化学计量比将质膜连接到细胞骨架。在唾液腺上皮细胞中,Ano1,ezrin和moesin / radixin在根尖共定位,而在HEK细胞中过表达moesin和Ano1会改变这两种蛋白的亚细胞定位。此外,对肌动蛋白的干扰RNA会修饰Ano1电流,而不会影响其表面表达水平。与Ano1相关的另一个网络包括SNARE和SM蛋白VAMP3,syntaxin 2和-4以及syntaxin结合蛋白munc18b和munc18c,它们是囊泡向质膜转运所必需的。 Ano1复合物中富含GTPases,Ca 2 + 结合蛋白,激酶和脂质相互作用蛋白等许多其他调节蛋白。这些数据提供了有关调节Ano1功能和转运至质膜极化域的机制的化学计量优先信息。

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