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Role of phosphorylated Thr-197 in the catalytic subunit of cAMP-dependent protein kinase

机译:磷酸化的Thr-197在cAMP依赖性蛋白激酶的催化亚基中的作用

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Protein phosphorylation of Thr-197 in the activation loop of the catalytic subunit (C-subunit) of cAMP-dependent protein kinase (PKA) is an essential step for its proper biological function. In order to explore the influences triggered by phosphoryiation of Thr-197, comparative molecular dynamics (MD) simulation studies with or without phosphate group on Thr-197 and Ser-338 were performed on the complex of C-subunit bound to ATP and two Mg2+ ions {C/Mg2ATP complex) and on the complex of C-subunit bound to substrate peptide (C/substrate complex). The results present a decreased flexibility of the activation loop in the phosphorylated state, because of several critical interactions formed by the phosphorylated Thr-197 with His-87, Arg-165, Lys-189 and Thr-195. The unphosphorylated activation loop does not block the substrate-binding site, which is in good agreement with experimental result. In unphos phorylated state, the crucial interaction between Thr-197and His-87 of C-helix does not exist, which eventually makes glycine-rich loop run away from its original position and displaces the phosphates group of ATP. We suggest that the reduction in rate of phosphoryl transfer may be caused by the displacement of γ-phosphate group that demolish phosphoryl transfer in-line mechanism,
机译:cAMP依赖性蛋白激酶(PKA)的催化亚基(C-亚基)激活环中的Thr-197蛋白磷酸化是其正常生物学功能的重要步骤。为了探讨Thr-197磷酸化所引发的影响,对结合或不结合磷酸基团的Thr-197和Ser-338进行了比较分子动力学(MD)模拟研究,研究了与ATP和两个Mg2 +结合的C亚基的复合物离子(C / Mg2ATP复合物)和结合到底物肽的C亚基复合物(C /底物复合物)上。由于磷酸化的Thr-197与His-87,Arg-165,Lys-189和Thr-195形成了几种关键的相互作用,因此结果表明磷酸化状态下激活环的柔性降低。未磷酸化的激活环不阻断底物结合位点,这与实验结果非常吻合。在未磷酸化的状态下,C-螺旋的Thr-197和His-87之间不存在关键的相互作用,最终使富含甘氨酸的环脱离其原始位置并取代了ATP的磷酸基团。我们认为,磷酰基转移速率的降低可能是由于γ-磷酸基团的置换破坏了磷酰基转移的内联机理,

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