Pericyte FAK negatively regulates Gas6/Axl signalling to suppress tumour angiogenesis and tumour growth

Tanguy Lechertier; Louise E. Reynolds; Hyojin Kim; Ana Rita Pedrosa; Jesús Gómez-Escudero; José M. Muñoz-Félix; Silvia Batista; Matthew Dukinfield; Fevzi Demircioglu; Ping Pui Wong; Kylie P. Matchett; Neil C. Henderson; Gabriela D’Amico; Maddy Parsons; Catherine Harwood; Pascal Meier; Kairbaan M. Hodivala-Dilke

doi:10.1038/s41467-020-16618-6

Nature Communications (Jun 2020)

Pericyte FAK negatively regulates Gas6/Axl signalling to suppress tumour angiogenesis and tumour growth

Tanguy Lechertier,
Louise E. Reynolds,
Hyojin Kim,
Ana Rita Pedrosa,
Jesús Gómez-Escudero,
José M. Muñoz-Félix,
Silvia Batista,
Matthew Dukinfield,
Fevzi Demircioglu,
Ping Pui Wong,
Kylie P. Matchett,
Neil C. Henderson,
Gabriela D’Amico,
Maddy Parsons,
Catherine Harwood,
Pascal Meier,
Kairbaan M. Hodivala-Dilke

Affiliations

Tanguy Lechertier: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Louise E. Reynolds: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Hyojin Kim: Cell Death & Inflammation, The Breast Cancer Now Toby Robins Research Centre, Institute of Cancer Research
Ana Rita Pedrosa: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Jesús Gómez-Escudero: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
José M. Muñoz-Félix: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Silvia Batista: Systems Oncology Group, Champalimaud Research, Champalimaud Centre for the Unknown Av. Brasília, Doca de Pedrouços
Matthew Dukinfield: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Fevzi Demircioglu: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Ping Pui Wong: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Kylie P. Matchett: Centre for Inflammation Research, The Queen’s Medical Research Institute, Edinburgh BioQuarter, University of Edinburgh
Neil C. Henderson: Centre for Inflammation Research, The Queen’s Medical Research Institute, Edinburgh BioQuarter, University of Edinburgh
Gabriela D’Amico: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre
Maddy Parsons: Nikon Imaging Centre@King’s, Randall Division of Cell and Molecular Biophysics, Kings College London
Catherine Harwood: Centre for Cell Biology and Cutaneous Research, Blizard Institute, Barts and The London School of Medicine and Dentistry, Queen Mary University of London
Pascal Meier: Cell Death & Inflammation, The Breast Cancer Now Toby Robins Research Centre, Institute of Cancer Research
Kairbaan M. Hodivala-Dilke: Centre for Tumour Biology, Barts Cancer Institute – a CR-UK Centre of Excellence, Queen Mary University of London, John Vane Science Centre

DOI: https://doi.org/10.1038/s41467-020-16618-6
Journal volume & issue: Vol. 11, no. 1
pp. 1 – 14

Abstract

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Abstract The overexpression of the protein tyrosine kinase, Focal adhesion kinase (FAK), in endothelial cells has implicated its requirement in angiogenesis and tumour growth, but how pericyte FAK regulates tumour angiogenesis is unknown. We show that pericyte FAK regulates tumour growth and angiogenesis in multiple mouse models of melanoma, lung carcinoma and pancreatic B-cell insulinoma and provide evidence that loss of pericyte FAK enhances Gas6-stimulated phosphorylation of the receptor tyrosine kinase, Axl with an upregulation of Cyr61, driving enhanced tumour growth. We further show that pericyte derived Cyr61 instructs tumour cells to elevate expression of the proangiogenic/protumourigenic transmembrane receptor Tissue Factor. Finally, in human melanoma we show that when 50% or more tumour blood vessels are pericyte-FAK negative, melanoma patients are stratified into those with increased tumour size, enhanced blood vessel density and metastasis. Overall our data uncover a previously unknown mechanism of tumour growth by pericytes that is controlled by pericyte FAK.

Published in Nature Communications

ISSN: 2041-1723 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Science
Website: https://www.nature.com/ncomms/

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