| Literature DB >> 31294477 |
Hong Jia1, Jagadeesh Janjanam1, Sharon C Wu1, Ruishan Wang1, Glendin Pano1, Marina Celestine1, Ophelie Martinot1, Hannah Breeze-Jones1, Georgia Clayton1, Cecile Garcin1, Abbas Shirinifard1, Ana Maria Zaske2, David Finkelstein3, Myriam Labelle1.
Abstract
Collagen linearization is a hallmark of aggressive tumors and a key pathogenic event that promotes cancer cell invasion and metastasis. Cell-generated mechanical tension has been proposed to contribute to collagen linearization in tumors, but it is unknown whether other mechanisms play prominent roles in this process. Here, we show that the secretome of cancer cells is by itself able to induce collagen linearization independently of cell-generated mechanical forces. Among the tumor cell-secreted factors, we find a key role in this process for the matricellular protein WISP1 (CCN4). Specifically, WISP1 directly binds to type I collagen to promote its linearization in vitro (in the absence of cells) and in vivo in tumors. Consequently, WISP1-induced type I collagen linearization facilitates tumor cell invasion and promotes spontaneous breast cancer metastasis, without significantly affecting gene expression. Furthermore, higher WISP1 expression in tumors from cancer patients correlates with faster progression to metastatic disease and poor prognosis. Altogether, these findings reveal a conceptually novel mechanism whereby pro-metastatic collagen linearization critically depends on a cancer cell-secreted factor.Entities:
Keywords: WISP1; breast cancer; collagen; invasion; metastasis
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Year: 2019 PMID: 31294477 PMCID: PMC6694215 DOI: 10.15252/embj.2018101302
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598