Cancer cell adaptation to hypoxia involves a HIF‐GPRC5A‐YAP axis

Alexander Greenhough; Clare Bagley; Kate J Heesom; David B Gurevich; David Gay; Mark Bond; Tracey J Collard; Chris Paraskeva; Paul Martin; Owen J Sansom; Karim Malik; Ann C Williams

doi:10.15252/emmm.201708699

EMBO Molecular Medicine (Nov 2018)

Cancer cell adaptation to hypoxia involves a HIF‐GPRC5A‐YAP axis

Alexander Greenhough,
Clare Bagley,
Kate J Heesom,
David B Gurevich,
David Gay,
Mark Bond,
Tracey J Collard,
Chris Paraskeva,
Paul Martin,
Owen J Sansom,
Karim Malik,
Ann C Williams

Affiliations

Alexander Greenhough: Cancer Research UK Colorectal Tumour Biology Group School of Cellular & Molecular Medicine Faculty of Life Sciences University of Bristol Bristol UK
Clare Bagley: Cancer Research UK Colorectal Tumour Biology Group School of Cellular & Molecular Medicine Faculty of Life Sciences University of Bristol Bristol UK
Kate J Heesom: Proteomics Facility Faculty of Life Sciences University of Bristol Bristol UK
David B Gurevich: School of Biochemistry Faculty of Life Sciences University of Bristol Bristol UK
David Gay: Cancer Research UK Beatson Institute Glasgow UK
Mark Bond: School of Clinical Sciences University of Bristol Bristol UK
Tracey J Collard: Cancer Research UK Colorectal Tumour Biology Group School of Cellular & Molecular Medicine Faculty of Life Sciences University of Bristol Bristol UK
Chris Paraskeva: Cancer Research UK Colorectal Tumour Biology Group School of Cellular & Molecular Medicine Faculty of Life Sciences University of Bristol Bristol UK
Paul Martin: School of Biochemistry Faculty of Life Sciences University of Bristol Bristol UK
Owen J Sansom: Cancer Research UK Beatson Institute Glasgow UK
Karim Malik: Cancer Epigenetics Laboratory School of Cellular & Molecular Medicine Faculty of Life Sciences University of Bristol Bristol UK
Ann C Williams: Cancer Research UK Colorectal Tumour Biology Group School of Cellular & Molecular Medicine Faculty of Life Sciences University of Bristol Bristol UK

DOI: https://doi.org/10.15252/emmm.201708699
Journal volume & issue: Vol. 10, no. 11
pp. n/a – n/a

Abstract

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Abstract Hypoxia is a hallmark of solid tumours and a key physiological feature distinguishing cancer from normal tissue. However, a major challenge remains in identifying tractable molecular targets that hypoxic cancer cells depend on for survival. Here, we used SILAC‐based proteomics to identify the orphan G protein‐coupled receptor GPRC5A as a novel hypoxia‐induced protein that functions to protect cancer cells from apoptosis during oxygen deprivation. Using genetic approaches in vitro and in vivo, we reveal HIFs as direct activators of GPRC5A transcription. Furthermore, we find that GPRC5A is upregulated in the colonic epithelium of patients with mesenteric ischaemia, and in colorectal cancers high GPRC5A correlates with hypoxia gene signatures and poor clinical outcomes. Mechanistically, we show that GPRC5A enables hypoxic cell survival by activating the Hippo pathway effector YAP and its anti‐apoptotic target gene BCL2L1. Importantly, we show that the apoptosis induced by GPRC5A depletion in hypoxia can be rescued by constitutively active YAP. Our study identifies a novel HIF‐GPRC5A‐YAP axis as a critical mediator of the hypoxia‐induced adaptive response and a potential target for cancer therapy.

Published in EMBO Molecular Medicine

ISSN: 1757-4676 (Print); 1757-4684 (Online)
Publisher: Springer Nature
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General); Science: Biology (General): Genetics
Website: https://www.embopress.org/journal/17574684

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Abstract

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