Macrophages induce malignant traits in mammary epithelium via IKKε/TBK1 kinases and the serine biosynthesis pathway

Ewa Wilcz‐Villega; Edward Carter; Alastair Ironside; Ruoyan Xu; Isabella Mataloni; Julie Holdsworth; William Jones; Rocío Moreno Béjar; Lukas Uhlik; Robert B Bentham; Susana A Godinho; Jesmond Dalli; Richard Grose; Gyorgy Szabadkai; Louise Jones; Kairbaan Hodivala‐Dilke; Katiuscia Bianchi

doi:10.15252/emmm.201910491

EMBO Molecular Medicine (Feb 2020)

Macrophages induce malignant traits in mammary epithelium via IKKε/TBK1 kinases and the serine biosynthesis pathway

Ewa Wilcz‐Villega,
Edward Carter,
Alastair Ironside,
Ruoyan Xu,
Isabella Mataloni,
Julie Holdsworth,
William Jones,
Rocío Moreno Béjar,
Lukas Uhlik,
Robert B Bentham,
Susana A Godinho,
Jesmond Dalli,
Richard Grose,
Gyorgy Szabadkai,
Louise Jones,
Kairbaan Hodivala‐Dilke,
Katiuscia Bianchi

Affiliations

Ewa Wilcz‐Villega: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Edward Carter: Centre for Tumour Biology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Alastair Ironside: Centre for Tumour Biology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Ruoyan Xu: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Isabella Mataloni: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Julie Holdsworth: Centre for Tumour Biology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
William Jones: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Rocío Moreno Béjar: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Lukas Uhlik: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Robert B Bentham: Department of Cell and Developmental Biology Consortium for Mitochondrial Research University College London London UK
Susana A Godinho: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Jesmond Dalli: Lipid Mediator Unit, Biochemical Pharmacology William Harvey Research Institute Barts and the London School of Medicine Queen Mary University of London London UK
Richard Grose: Centre for Tumour Biology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Gyorgy Szabadkai: Department of Cell and Developmental Biology Consortium for Mitochondrial Research University College London London UK
Louise Jones: Centre for Tumour Biology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Kairbaan Hodivala‐Dilke: Centre for Tumour Biology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK
Katiuscia Bianchi: Centre for Molecular Oncology Barts Cancer Institute John Vane Science Centre Queen Mary University of London London UK

DOI: https://doi.org/10.15252/emmm.201910491
Journal volume & issue: Vol. 12, no. 2
pp. n/a – n/a

Abstract

Read online

Abstract During obesity, macrophages infiltrate the breast tissue leading to low‐grade chronic inflammation, a factor considered responsible for the higher risk of breast cancer associated with obesity. Here, we formally demonstrate that breast epithelial cells acquire malignant properties when exposed to medium conditioned by macrophages derived from human healthy donors. These effects were mediated by the breast cancer oncogene IKKε and its downstream target—the serine biosynthesis pathway as demonstrated by genetic or pharmacological tools. Furthermore, amlexanox, an FDA‐approved drug targeting IKKε and its homologue TBK1, delayed in vivo tumour formation in a combined genetic mouse model of breast cancer and high‐fat diet‐induced obesity/inflammation. Finally, in human breast cancer tissues, we validated the link between inflammation–IKKε and alteration of cellular metabolism. Altogether, we identified a pathway connecting obesity‐driven inflammation to breast cancer and a potential therapeutic strategy to reduce the risk of breast cancer associated with obesity.

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

About the journal

Abstract

Keywords