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The chemical diversity and structure-based discovery of allosteric modulators for the PIF-pocket of protein kinase PDK1

机译:化学激酶和基于结构的蛋白质激酶PDK1 PIF口袋变构调节剂的发现。

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摘要

Phosphoinositide-dependent protein kinase-1 (PDK1) is an important protein in mediating the PI3K-AKT pathway and is thus identified as a promising target. The catalytic activity of PDK1 is tightly regulated by allosteric modulators, which bind to the PDK1 Interacting Fragment (PIF) pocket of the kinase domain that is topographically distinct from the orthosteric, ATP binding site. Allosteric modulators by attaching to the less conserved PIF-pocket have remarkable advantages such as higher selectivity, less side effect, and lower toxicity. Targeting allosteric PIF-pocket of PDK1 has become the focus of recent attention. In this review, we summarise the current advances in the structure-based discovery of PDK1 allosteric modulators. We will first present the three-dimensional structure of PDK1 and illustrate the allosteric regulatory mechanism of PDK1 through the modulation of the PIF-pocket. Then, the recent advances of PDK1 allosteric modulators targeting the PIF-pocket will be recapitulated detailly according to the structural similarity of allosteric modulators.
机译:磷酸肌醇依赖性蛋白激酶-1(PDK1)是介导PI3K-AKT途径的重要蛋白,因此被确定为有希望的靶标。 PDK1的催化活性受到变构调节剂的严格调节,该变构调节剂与激酶结构域的PDK1相互作用片段(PIF)口袋结合,该口袋在地形上与正构ATP结合位点不同。通过与保守程度较低的PIF口袋相连,变构调节剂具有显着的优势,例如更高的选择性,更少的副作用和更低的毒性。靶向PDK1的变构PIF口袋已成为近期关注的焦点。在这篇综述中,我们总结了PDK1变构调节剂在基于结构的发现中的最新进展。我们将首先介绍PDK1的三维结构,并通过PIF口袋的调制来说明PDK1的变构调节机制。然后,将根据变构调节剂的结构相似性,详细概述靶向PIF口袋的PDK1变构调节剂的最新进展。

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