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A Complex Interplay of Anionic Phospholipid Binding Regulates 3'-Phosphoinositide-Dependent-Kinase-1 Homodimer Activation

Authors :
Ministerio de Economía y Competitividad (España)
Centre National de la Recherche Scientifique (France)
Larijani, B. [0000-0003-4735-1169]
Requejo-Isidro, José [0000-0002-2465-6288]
Heras-Martínez, Gloria de las
Calleja, V.
Bailly, R.
Dessolin, J.
Larijani, Banafshé
Requejo-Isidro, José
Ministerio de Economía y Competitividad (España)
Centre National de la Recherche Scientifique (France)
Larijani, B. [0000-0003-4735-1169]
Requejo-Isidro, José [0000-0002-2465-6288]
Heras-Martínez, Gloria de las
Calleja, V.
Bailly, R.
Dessolin, J.
Larijani, Banafshé
Requejo-Isidro, José
Publication Year :
2019

Abstract

3'-Phosphoinositide-dependent-Kinase-1(PDK1) is a master regulator whereby its PI3- kinase-dependent dysregulation in human pathologies is well documented. Understanding the direct role for Ptdlns(3,4,5)P-3 and other anionic phospholipids in the regulation of PDK1 conformational dynamics and its downstream activation remains incomplete. Using advanced quantitative-time-resolved imaging (Fluorescence Lifetime Imaging and Fluorescence Correlation Spectroscopy) and molecular modelling, we show an interplay of antagonistic binding effects of Ptdlns(3,4,5)P-3 and other anionic phospholipids, regulating activated PDK1 homodimers. We demonstrate that phosphatidylserine maintains PDK1 in an inactive conformation. The dysregulation of the PI3K pathway affects the spatio-temporal and conformational dynamics of PDK1 and the activation of its downstream substrates. We have established a new anionic-phospholipid-dependent model for PDK1 regulation, depicting the conformational dynamics of multiple homodimer states. We show that the dysregulation of the PI3K pathway perturbs equilibrium between the PDK1 homodimer conformations. Our findings provide a role for the PtdSer binding site and its previously unrewarding role in PDK1 downregulation, suggesting a possible therapeutic strategy where the constitutively active dimer conformer of PDK1 may be rendered inactive by small molecules that drive it to its PtdSer-bound conformer.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1286549220
Document Type :
Electronic Resource