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MAPL is a new mitochondrial SUMO E3 ligase that regulates mitochondrial fission

机译:MAPL是一种新的线粒体SUMO E3连接酶可调节线粒体裂变

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摘要

The modification of proteins by the small ubiquitin-like modifier (SUMO) is known to regulate an increasing array of cellular processes. SUMOylation of the mitochondrial fission GTPase dynamin-related protein 1 (DRP1) stimulates mitochondrial fission, suggesting that SUMOylation has an important function in mitochondrial dynamics. The conjugation of SUMO to its substrates requires a regulatory SUMO E3 ligase; however, so far, none has been functionally associated with the mitochondria. By using biochemical assays, overexpression and RNA interference experiments, we characterized the mitochondrial-anchored protein ligase (MAPL) as the first mitochondrial-anchored SUMO E3 ligase. Furthermore, we show that DRP1 is a substrate for MAPL, providing a direct link between MAPL and the fission machinery. Importantly, the large number of unidentified mitochondrial SUMO targets suggests a global role for SUMOylation in mitochondrial function, placing MAPL as a crucial component in the regulation of multiple conjugation events.
机译:已知通过小泛素样修饰剂(SUMO)修饰蛋白质可调节越来越多的细胞过程。线粒体裂变的SUMOylation GTPase动力蛋白相关蛋白1(DRP1)刺激线粒体裂变,表明SUMOylation在线粒体动力学中具有重要作用。 SUMO与其底物的缀合需要调节的SUMO E3连接酶。然而,到目前为止,还没有功能与线粒体相关。通过使用生化测定,过表达和RNA干扰实验,我们将线粒体锚定蛋白连接酶(MAPL)表征为第一个线粒体锚定的SUMO E3连接酶。此外,我们表明DRP1是MAPL的底物,提供了MAPL和裂变机械之间的直接联系。重要的是,大量未确定的线粒体SUMO靶标提示SUMOylation在线粒体功能中具有全球性作用,这使MAPL成为调控多种共轭事件的重要组成部分。

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