Differential epigenetic reprogramming in response to specific endocrine therapies promotes cholesterol biosynthesis and cellular invasion
Data(s) |
27/11/2015
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Resumo |
Endocrine therapies target the activation of the oestrogen receptor alpha (ERα) via distinct mechanisms, but it is not clear whether breast cancer cells can adapt to treatment using drug-specific mechanisms. Here we demonstrate that resistance emerges via drug-specific epigenetic reprogramming. Resistant cells display a spectrum of phenotypical changes with invasive phenotypes evolving in lines resistant to the aromatase inhibitor (AI). Orthogonal genomics analysis of reprogrammed regulatory regions identifies individual drug-induced epigenetic states involving large topologically associating domains (TADs) and the activation of super-enhancers. AI-resistant cells activate endogenous cholesterol biosynthesis (CB) through stable epigenetic activation in vitro and in vivo. Mechanistically, CB sparks the constitutive activation of oestrogen receptors alpha (ERα) in AI-resistant cells, partly via the biosynthesis of 27-hydroxycholesterol. By targeting CB using statins, ERα binding is reduced and cell invasion is prevented. Epigenomic-led stratification can predict resistance to AI in a subset of ERα-positive patients |
Formato |
text |
Identificador |
http://centaur.reading.ac.uk/48345/1/ncomms10044.pdf Nguyen, V. T.M., Barozzi, I., Faronata, M., Lombardo, Y., Steel, J. H., Patel, N., Darbre, P. <http://centaur.reading.ac.uk/view/creators/90000451.html>, Castellano, L., Gyorffy, B., Woodley, L., Meira, A., Patten, D. K., Vircillo, V., Periyasamy, M., Ali, S., Frige, G., Minucci, S., Coombes, R. C. and Magnani, L. (2015) Differential epigenetic reprogramming in response to specific endocrine therapies promotes cholesterol biosynthesis and cellular invasion. Nature Communications, 6. 10044. ISSN 2041-1723 doi: 10.1038/ncomms10044 <http://dx.doi.org/10.1038/ncomms10044> |
Idioma(s) |
en |
Publicador |
Nature Publishing Group |
Relação |
http://centaur.reading.ac.uk/48345/ creatorInternal Darbre, Philippa 10.1038/ncomms10044 |
Direitos |
cc_by_4 |
Tipo |
Article PeerReviewed |