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Fibroblast subtypes define a metastatic matrisome in breast cancer
Heather M. Brechbuhl, Alexander S. Barrett, Etana Kopin, Jaime C. Hagen, Amy L. Han, Austin E. Gillen, Jessica Finlay-Schultz, Diana M. Cittelly, Philip Owens, Kathryn B. Horwitz, Carol A. Sartorius, Kirk Hansen, Peter Kabos
Heather M. Brechbuhl, Alexander S. Barrett, Etana Kopin, Jaime C. Hagen, Amy L. Han, Austin E. Gillen, Jessica Finlay-Schultz, Diana M. Cittelly, Philip Owens, Kathryn B. Horwitz, Carol A. Sartorius, Kirk Hansen, Peter Kabos
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Research Article Oncology

Fibroblast subtypes define a metastatic matrisome in breast cancer

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Abstract

Small primary breast cancers can show surprisingly high potential for metastasis. Clinical decision-making for tumor aggressiveness, including molecular profiling, relies primarily on analysis of the cancer cells. Here we show that this analysis is insufficient — that the stromal microenvironment of the primary tumor plays a key role in tumor cell dissemination and implantation at distant sites. We previously described 2 cancer-associated fibroblasts (CAFs) that either express (CD146+) or lack (CD146–) CD146 (official symbol MCAM, alias MUC18). We now find that when mixed with human breast cancer cells, each fibroblast subtype determines the fate of cancer cells: CD146– fibroblasts promoted increased metastasis compared with CD146+ fibroblasts. Potentially novel quantitative and qualitative proteomic analyses showed that CD146+ CAFs produced an environment rich in basement membrane proteins, while CD146– CAFs exhibited increases in fibronectin 1, lysyl oxidase, and tenascin C, all overexpressed in aggressive disease. We also show clinically that CD146– CAFs predicted for likelihood of lymph node involvement even in small primary tumors (<5 cm). Clearly small tumors enriched for CD146– CAFs require aggressive treatments.

Authors

Heather M. Brechbuhl, Alexander S. Barrett, Etana Kopin, Jaime C. Hagen, Amy L. Han, Austin E. Gillen, Jessica Finlay-Schultz, Diana M. Cittelly, Philip Owens, Kathryn B. Horwitz, Carol A. Sartorius, Kirk Hansen, Peter Kabos

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Figure 9

MCF-7 spheroid invasion fronts expressing TNC have significantly more p-ERK expression.

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MCF-7 spheroid invasion fronts expressing TNC have significantly more p-...
MCF-7 spheroids were cocultured with CD146– CAFs (HS5) expressing (A) control shRNA (shCont) or (B) shRNA against TNC (shTNC88). IHC for p-ERK (pERK, blue) and TNC (brown) in 3 representative spheroids and counterstained with nuclear fast red. Insets are marked by a blue box. (C) Intensity scores on a scale of 1 to 3 (1, minimal staining; 2, moderate staining; 3, intense staining) for p-ERK and TNC. Per spheroid 4–6 serial images were scored, with n = 3 spheroids per group. Scale bars: 100 mm. ****P < 0.0001; statistics were completed using an ordinary 1-way ANOVA followed by Tukey’s multiple-comparisons test.

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