PH domain-mediated autoinhibition and oncogenic activation of Akt

Hwan Bae; Thibault Viennet; Eunyoung Park; Nam Chu; Antonieta Salguero; Michael J. Eck; Haribabu Arthanari; Philip A. Cole

doi:10.7554/eLife.80148

PH domain-mediated autoinhibition and oncogenic activation of Akt

Hwan Bae, Thibault Viennet, Eunyoung Park, Nam Chu, Antonieta Salguero, Michael J. Eck, Haribabu Arthanari, Philip A. Cole

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6 Scopus citations

Abstract

Akt is a Ser/Thr protein kinase that plays a central role in metabolism and cancer. Regulation of Akt’s activity involves an autoinhibitory intramolecular interaction between its pleck-strin homology (PH) domain and its kinase domain that can be relieved by C-tail phosphorylation. PH domain mutant E17K Akt is a well-established oncogene. Previously, we reported that the conformation of autoinhibited Akt may be shifted by small molecule allosteric inhibitors limiting the mechanistic insights from existing X-ray structures that have relied on such compounds (Chu et al., 2020). Here, we discover unexpectedly that a single mutation R86A Akt exhibits intensified autoin-hibitory features with enhanced PH domain-kinase domain affinity. Structural and biochemical analysis uncovers the importance of a key interaction network involving Arg86, Glu17, and Tyr18 that controls Akt conformation and activity. Our studies also shed light on the molecular basis for E17K Akt activation as an oncogenic driver.

Original language	English
Article number	e80148
Journal	eLife
Volume	11
DOIs	https://doi.org/10.7554/eLife.80148
State	Published - 2022

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title = "PH domain-mediated autoinhibition and oncogenic activation of Akt",

abstract = "Akt is a Ser/Thr protein kinase that plays a central role in metabolism and cancer. Regulation of Akt{\textquoteright}s activity involves an autoinhibitory intramolecular interaction between its pleck-strin homology (PH) domain and its kinase domain that can be relieved by C-tail phosphorylation. PH domain mutant E17K Akt is a well-established oncogene. Previously, we reported that the conformation of autoinhibited Akt may be shifted by small molecule allosteric inhibitors limiting the mechanistic insights from existing X-ray structures that have relied on such compounds (Chu et al., 2020). Here, we discover unexpectedly that a single mutation R86A Akt exhibits intensified autoin-hibitory features with enhanced PH domain-kinase domain affinity. Structural and biochemical analysis uncovers the importance of a key interaction network involving Arg86, Glu17, and Tyr18 that controls Akt conformation and activity. Our studies also shed light on the molecular basis for E17K Akt activation as an oncogenic driver.",

author = "Hwan Bae and Thibault Viennet and Eunyoung Park and Nam Chu and Antonieta Salguero and Eck, {Michael J.} and Haribabu Arthanari and Cole, {Philip A.}",

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T1 - PH domain-mediated autoinhibition and oncogenic activation of Akt

AU - Bae, Hwan

AU - Viennet, Thibault

AU - Park, Eunyoung

AU - Chu, Nam

AU - Salguero, Antonieta

AU - Eck, Michael J.

AU - Arthanari, Haribabu

AU - Cole, Philip A.

PY - 2022

Y1 - 2022

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AB - Akt is a Ser/Thr protein kinase that plays a central role in metabolism and cancer. Regulation of Akt’s activity involves an autoinhibitory intramolecular interaction between its pleck-strin homology (PH) domain and its kinase domain that can be relieved by C-tail phosphorylation. PH domain mutant E17K Akt is a well-established oncogene. Previously, we reported that the conformation of autoinhibited Akt may be shifted by small molecule allosteric inhibitors limiting the mechanistic insights from existing X-ray structures that have relied on such compounds (Chu et al., 2020). Here, we discover unexpectedly that a single mutation R86A Akt exhibits intensified autoin-hibitory features with enhanced PH domain-kinase domain affinity. Structural and biochemical analysis uncovers the importance of a key interaction network involving Arg86, Glu17, and Tyr18 that controls Akt conformation and activity. Our studies also shed light on the molecular basis for E17K Akt activation as an oncogenic driver.

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JO - eLife

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PH domain-mediated autoinhibition and oncogenic activation of Akt

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