| Literature DB >> 26290412 |
Bo Ri Seo1, Priya Bhardwaj2, Siyoung Choi1, Jacqueline Gonzalez1, Roberto C Andresen Eguiluz3, Karin Wang4, Sunish Mohanan5, Patrick G Morris6, Baoheng Du2, Xi K Zhou7, Linda T Vahdat2, Akanksha Verma8, Olivier Elemento8, Clifford A Hudis6, Rebecca M Williams1, Delphine Gourdon3, Andrew J Dannenberg2, Claudia Fischbach9.
Abstract
Obesity and extracellular matrix (ECM) density are considered independent risk and prognostic factors for breast cancer. Whether they are functionally linked is uncertain. We investigated the hypothesis that obesity enhances local myofibroblast content in mammary adipose tissue and that these stromal changes increase malignant potential by enhancing interstitial ECM stiffness. Indeed, mammary fat of both diet- and genetically induced mouse models of obesity were enriched for myofibroblasts and stiffness-promoting ECM components. These differences were related to varied adipose stromal cell (ASC) characteristics because ASCs isolated from obese mice contained more myofibroblasts and deposited denser and stiffer ECMs relative to ASCs from lean control mice. Accordingly, decellularized matrices from obese ASCs stimulated mechanosignaling and thereby the malignant potential of breast cancer cells. Finally, the clinical relevance and translational potential of our findings were supported by analysis of patient specimens and the observation that caloric restriction in a mouse model reduces myofibroblast content in mammary fat. Collectively, these findings suggest that obesity-induced interstitial fibrosis promotes breast tumorigenesis by altering mammary ECM mechanics with important potential implications for anticancer therapies.Entities:
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Year: 2015 PMID: 26290412 PMCID: PMC4837896 DOI: 10.1126/scitranslmed.3010467
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956