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Structural and Dynamic Effects of PTEN C-Terminal Tail Phosphorylation

Iris Nira Smith, Jennifer E. Dawson, James Krieger, Stetson Thacker, İvet Bahar, Charis Eng

2022Journal of Chemical Information and Modeling19 citationsDOIOpen Access PDF

Abstract

) tumor suppressor gene encodes a tightly regulated dual-specificity phosphatase that serves as the master regulator of PI3K/AKT/mTOR signaling. The carboxy-terminal tail (CTT) is key to regulation and harbors multiple phosphorylation sites (Ser/Thr residues 380-385). CTT phosphorylation suppresses the phosphatase activity by inducing a stable, closed conformation. However, little is known about the mechanisms of phosphorylation-induced CTT-deactivation dynamics. Using explicit solvent microsecond molecular dynamics simulations, we show that CTT phosphorylation leads to a partially collapsed conformation, which alters the secondary structure of PTEN and induces long-range conformational rearrangements that encompass the active site. The active site rearrangements prevent localization of PTEN to the membrane, precluding lipid phosphatase activity. Notably, we have identified phosphorylation-induced allosteric coupling between the interdomain region and a hydrophobic site neighboring the active site in the phosphatase domain. Collectively, the results provide a mechanistic understanding of CTT phosphorylation dynamics and reveal potential druggable allosteric sites in a previously believed clinically undruggable protein.

Topics & Concepts

PTENTensinPhosphorylationPhosphataseAllosteric regulationChemistryProtein phosphatase 2Cell biologyBiologyProtein kinase BPI3K/AKT/mTOR pathwayBiochemistrySignal transductionEnzymePI3K/AKT/mTOR signaling in cancerProtein Kinase Regulation and GTPase SignalingCoagulation, Bradykinin, Polyphosphates, and Angioedema
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