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Implanted adipose progenitor cells as physicochemical regulators of breast cancer

Cornell Affiliated Author(s)

Author

E.M. Chandler
B.R. Seo
J.P. Califano
R.C. Eguiluz
J.S. Lee
C.J. Yoon
D.T. Tims
J.X. Wang
L. Cheng
S. Mohanan
M.R. Buckley
Itai Cohen
A.Y. Nikitin
R.M. Williams
D. Gourdon
C.A. Reinhart-King
C. Fischbach

Abstract

Multipotent adipose-derived stem cells (ASCs) are increasingly used for regenerative purposes such as soft tissue reconstruction following mastectomy; however, the ability of tumors to commandeer ASC functions to advance tumor progression is not well understood. Through the integration of physical sciences and oncology approaches we investigated the capability of tumor-derived chemical and mechanical cues to enhance ASC-mediated contributions to tumor stroma formation. Our results indicate that soluble factors from breast cancer cells inhibit adipogenic differentiation while increasing proliferation, proangiogenic factor secretion, and myofibroblastic differentiation of ASCs. This altered ASC phenotype led to varied extracellular matrix (ECM) deposition and contraction thereby enhancing tissue stiffness, a characteristic feature of breast tumors. Increased stiffness, in turn, facilitated changes in ASC behavior similar to those observed with tumor-derived chemical cues. Orthotopic mouse studies further confirmed the pathological relevance of ASCs in tumor progression and stiffness in vivo. In summary, altered ASC behavior can promote tumorigenesis and, thus, their implementation for regenerative therapy should be carefully considered in patients previously treated for cancer.

Date Published

Journal

Proceedings of the National Academy of Sciences of the United States of America

Volume

109

Issue

25

Number of Pages

9786-9791,

URL

https://www.scopus.com/inward/record.uri?eid=2-s2.0-84862543399&doi=10.1073%2fpnas.1121160109&partnerID=40&md5=d3151d192c685a5899c522306e32c99f

DOI

10.1073/pnas.1121160109

Research Area

Group (Lab)

Itai Cohen Group

Funding Source

RC1CA146065

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