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Statins mediate anti- and pro-tumourigenic functions by remodelling the tumour microenvironment

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journal contribution
posted on 2022-03-09, 06:16 authored by T Kamata, EA Dujaily, S Alhamad, TY So, O Margaritaki, S Giblett, JH Pringle, J Le Quesne, C Pritchard
Anti-cancer properties of statins are controversial and possibly context dependent. Recent pathology/epidemiology studies of human lung adenocarcinoma showed reduced pro-tumourigenic macrophages associated with a shift to lower-grade tumours amongst statin users but, paradoxically, worse survival compared with that of non-users. To investigate the mechanisms involved, we have characterised mouse lung adenoma/adenocarcinoma models treated with atorvastatin. Here, we show that atorvastatin suppresses premalignant disease by inhibiting the recruitment of pro-tumourigenic macrophages to the tumour microenvironment, manifested in part by suppression of Rac-mediated CCR1 ligand secretion. However, prolonged atorvastatin treatment leads to drug resistance and progression of lung adenomas into invasive disease. Pathological progression is not driven by acquisition of additional driver mutations or immunoediting/evasion but is associated with stromal changes including the development of desmoplastic stroma containing Gr1+ myeloid cells and tertiary lymphoid structures. These findings show that any chemopreventive functions of atorvastatin in lung adenocarcinoma are overridden by stromal remodelling in the long term, thus providing mechanistic insight into the poor survival of lung adenocarcinoma patients with statin use.

Funding

Cancer Research UK programme grant C1362/A13083

Leicester Wellcome Trust Institutional Strategic Support Fund

History

Citation

Dis Model Mech (2022) 15 (2): dmm049148.

Author affiliation

Leicester Cancer Research Centre, University of Leicester

Version

  • VoR (Version of Record)

Published in

DMM Disease Models and Mechanisms

Volume

15

Issue

2

Publisher

The Company of Biologists

issn

1754-8403

eissn

1754-8411

Acceptance date

2021-11-05

Copyright date

2022

Available date

2022-03-09

Language

eng

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