Molecular and Structural Biology Division, CSIR- Central Drug Research Institute, Sector 10, Jankipuram Extension, Sitapur Road, Lucknow, 226031, India.
Molecular and Structural Biology Division, CSIR- Central Drug Research Institute, Sector 10, Jankipuram Extension, Sitapur Road, Lucknow, 226031, India.
Eur J Cell Biol. 2018 May;97(4):300-307. doi: 10.1016/j.ejcb.2018.04.006. Epub 2018 Apr 20.
Mammalian Lst8 interacts with the kinase domain of mTOR and stabilizes its interaction with Raptor regulating cell growth through the mTOR-S6K1 signalling pathway. Fission yeast Wat1, an ortholog of mammalian Lst8 is also an essential component of TOR complex 1 (TORC1) and TOR Complex 2 (TORC2) that control protein kinases essential for metabolic pathways. Here, we show that in response to osmotic stress, the Wat1 protein undergoes hyper-phosphorylation at S116 position. Wat1 interacts with the C-terminal region of Tor1 that also contain kinase domain. Co-immunoprecipitation and molecular modelling studies suggest that Wat1-Tor1 interaction is stabilized by FATC domain of Tor1 protein present at the C-terminal region. We have also demonstrated a physical interaction of Wat1 with Gad8, an AGC family protein kinase that is dependent on phosphorylation of Wat1 at S116 residue. Wat1 phosphorylation is required for the maintenance of vacuolar integrity and sexual differentiation. Collectively, our study reveals Wat1 phosphorylation regulates Gad8 function in a manner dependent on Tor1 interaction.
哺乳动物 Lst8 与 mTOR 的激酶结构域相互作用,并通过 mTOR-S6K1 信号通路稳定其与 Raptor 的相互作用,从而调节细胞生长。裂殖酵母 Wat1 是哺乳动物 Lst8 的同源物,也是 TOR 复合物 1(TORC1)和 TOR 复合物 2(TORC2)的必需组成部分,这些复合物控制着代谢途径中必需的蛋白激酶。在这里,我们表明 Wat1 蛋白在 S116 位置发生过度磷酸化,以响应渗透压胁迫。Wat1 与 Tor1 的 C 末端区域相互作用,该区域还包含激酶结构域。共免疫沉淀和分子建模研究表明,Wat1-Tor1 相互作用由 Tor1 蛋白 C 末端的 FATC 结构域稳定。我们还证明了 Wat1 与 Gad8 的物理相互作用,Gad8 是一种 AGC 家族蛋白激酶,依赖于 Wat1 在 S116 残基上的磷酸化。Wat1 磷酸化对于液泡完整性和有性分化的维持是必需的。总之,我们的研究表明 Wat1 磷酸化调节 Gad8 功能,这种调节方式依赖于 Tor1 的相互作用。
