Modulation of the substrate specificity of the kinase PDK1 by distinct conformations of the full- length protein

被引:8
作者
Sacerdoti, Mariana [1 ]
Gross, Lissy Z. F. [1 ]
Riley, Andrew M. [2 ]
Zehnder, Karin [3 ]
Ghode, Abhijeet [4 ]
Klinke, Sebastian [5 ,6 ]
Anand, Ganesh Srinivasan [4 ,7 ]
Paris, Kristina [8 ,9 ]
Winkel, Angelika [3 ]
Herbrand, Amanda K. [3 ]
Godage, H. Yasmin [10 ]
Cozier, Gyles E. [10 ]
Suss, Evelyn [3 ]
Schulze, Joerg O. [3 ]
Pastor-Flores, Daniel [3 ,11 ]
Bollini, Mariela [12 ]
Cappellari, Maria Victoria [12 ]
Svergun, Dmitri [13 ]
Graewert, Melissa A. [13 ]
Aramendia, Pedro F. [12 ,14 ]
Leroux, Alejandro E. [1 ]
Potter, Barry V. L. [2 ,10 ]
Camacho, Carlos J. [8 ]
Biondi, Ricardo M. [1 ,3 ,15 ,16 ]
机构
[1] Inst Invest Biomed Buenos Aires IBioBA, CONICET Partner Inst Max Planck Soc, C1425FQD, Buenos Aires, DF, Argentina
[2] Univ Oxford, Dept Pharmacol, Med Chem & Drug Discovery, Mansfield Rd, Oxford OX1 3QT, England
[3] Univ Klinikum Frankfurt, Dept Internal Med 1, Theodor Stern Kai 7, D-60590 Frankfurt, Germany
[4] Natl Univ Singapore, Biol Sci, Singapore 119077, Singapore
[5] Consejo Nacl Invest Cient & Tecn, IIBBA, Fdn Inst Leloir, C1405BWE, Buenos Aires, DF, Argentina
[6] Plataforma Argentina Biol Estruct & Metabol PLAB, C1405BWE, Buenos Aires, DF, Argentina
[7] Penn State Univ, Huck Inst Life Sci, Dept Chem, 104 Chem Bldg, University Pk, PA 16802 USA
[8] Univ Pittsburgh, Dept Computat & Syst Biol, Pittsburgh, PA 15260 USA
[9] Univ Pittsburgh, Dept Stat, WWPH 1821, Pittsburgh, PA 15213 USA
[10] Univ Bath, Dept Life Sci, Wolfson Lab Med Chem, Bath BA2 7AY, Avon, England
[11] KBI Biopharm, Technol Laan 8, B-3001 Leuven, Belgium
[12] Consejo Nacl Invest Cient & Tecn, Ctr Invest Bionanociencias Elizabeth Jares Erijma, C1425FQD, Buenos Aires, DF, Argentina
[13] European Mol Biol Lab EMBL, Hamburg Unit, D-22607 Hamburg, Germany
[14] Univ Buenos Aires, Dept Quim Inorgan Analit & Quim Fis, FCEN, C1428EHA, Buenos Aires, DF, Argentina
[15] DKTK German Canc Consortium DKTK, Frankfurt, Germany
[16] German Canc Res Ctr, D-69120 Heidelberg, Germany
基金
欧盟地平线“2020”; 英国惠康基金;
关键词
PHOSPHOINOSITIDE-DEPENDENT KINASE; MOLECULAR-DYNAMICS SIMULATIONS; SMALL-ANGLE SCATTERING; X-RAY-SCATTERING; DOCKING-SITE; PH DOMAIN; INOSITOL PENTAKISPHOSPHATE; BINDING POCKET; AGC KINASES; C ISOZYMES;
D O I
10.1126/scisignal.add3184
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The activation of at least 23 different mammalian kinases requires the phosphorylation of their hydrophobic motifs by the kinase PDK1. A linker connects the phosphoinositide-binding PH domain to the catalytic domain, which contains a docking site for substrates called the PIF pocket. Here, we used a chemical biology approach to show that PDK1 existed in equilibrium between at least three distinct conformations with differing substrate specificities. The inositol polyphosphate derivative HYG8 bound to the PH domain and disrupted PDK1 dimerization by stabilizing a monomeric conformation in which the PH domain associated with the cat-alytic domain and the PIF pocket was accessible. In the absence of lipids, HYG8 potently inhibited the phosphor-ylation of Akt (also termed PKB) but did not affect the intrinsic activity of PDK1 or the phosphorylation of SGK, which requires docking to the PIF pocket. In contrast, the small-molecule valsartan bound to the PIF pocket and stabilized a second distinct monomeric conformation. Our study reveals dynamic conformations of full-length PDK1 in which the location of the linker and the PH domain relative to the catalytic domain determines the selective phosphorylation of PDK1 substrates. The study further suggests new approaches for the design of drugs to selectively modulate signaling downstream of PDK1.
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页数:21
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