The Oncogene AAMDC Links PI3K-AKT-mTOR Signaling with Metabolic Reprograming in Estrogen Receptor-positive Breast Cancer

Overview

Journal Nat Commun

Specialty Biology

Date 2021 Mar 27

PMID 33772001

Citations 16

Authors

Emily Golden

Rabab Rashwan

Eleanor A Woodward

Agustin Sgro

Edina Wang

Anabel Sorolla

Charlene Waryah

Wan Jun Tie

Elisabet Cuyas

Magdalena Ratajska

Iwona Kardas

Piotr Kozlowski

Elizabeth K M Johnstone

Heng B See

Ciara Duffy

Jeremy Parry

Kim A Lagerborg

Piotr Czapiewski

Javier A Menendez

Adam Gorczynski

Bartosz Wasag

Kevin D G Pfleger

Christina Curtis

Bum-Kyu Lee

Jonghwan Kim

Joseph Cursons

Nathan J Pavlos

Wojciech Biernat

Mohit Jain

Andrew J Woo

Andrew Redfern

Pilar Blancafort

Affiliations

Soon will be listed here.

Abstract

Adipogenesis associated Mth938 domain containing (AAMDC) represents an uncharacterized oncogene amplified in aggressive estrogen receptor-positive breast cancers. We uncover that AAMDC regulates the expression of several metabolic enzymes involved in the one-carbon folate and methionine cycles, and lipid metabolism. We show that AAMDC controls PI3K-AKT-mTOR signaling, regulating the translation of ATF4 and MYC and modulating the transcriptional activity of AAMDC-dependent promoters. High AAMDC expression is associated with sensitization to dactolisib and everolimus, and these PI3K-mTOR inhibitors exhibit synergistic interactions with anti-estrogens in IntClust2 models. Ectopic AAMDC expression is sufficient to activate AKT signaling, resulting in estrogen-independent tumor growth. Thus, AAMDC-overexpressing tumors may be sensitive to PI3K-mTORC1 blockers in combination with anti-estrogens. Lastly, we provide evidence that AAMDC can interact with the RabGTPase-activating protein RabGAP1L, and that AAMDC, RabGAP1L, and Rab7a colocalize in endolysosomes. The discovery of the RabGAP1L-AAMDC assembly platform provides insights for the design of selective blockers to target malignancies having the AAMDC amplification.

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