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PIKKing on PKB: regulation of PKB activity by phosphorylation

机译:在PKB上进行PIKKing:通过磷酸化调节PKB活性

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摘要

Ser/Thr protein kinase PKB/Akt is a key regulator of a wide range of cellular processes including growth, proliferation and survival. PKB is clearly a crucial signaling molecule and extensive research efforts aim to understand its regulation and action. Recent studies of the regulation of PKB activity by hydrophobic motif phosphorylation have yielded several exciting findings about members of the PI3-kinase-like family of kinases (PIKKs) acting as PKB regulators. Mammalian target of rapamycin complex 2 (mTORC2) and DNA-dependent protein kinase (DNA-PK) can both phosphorylate Ser473 and activate PKB. This present review concerns PKB regulation by mTORC2 and DNA-PK in a stimulus-dependent and context-dependent manner and the possible implications of this for PKB activity, substrate specificity and therapeutic intervention.
机译:Ser / Thr蛋白激酶PKB / Akt是包括生长,增殖和存活在内的多种细胞过程的关键调节剂。 PKB显然是至关重要的信号分子,广泛的研究工作旨在了解其调节和作用。通过疏水基序磷酸化对PKB活性进行调节的最新研究已经获得了有关PI3激酶样家族激酶(PIKK)充当PKB调节剂的成员的一些令人兴奋的发现。雷帕霉素复合物2(mTORC2)和DNA依赖性蛋白激酶(DNA-PK)的哺乳动物靶标都可以磷酸化Ser473并激活PKB。本综述涉及mTORC2和DNA-PK对PKB的调控,其依赖于刺激和上下文,并且可能对PKB活性,底物特异性和治疗干预产生潜在影响。

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