| Literature DB >> 32045383 |
Heather M Brechbuhl1, Alexander S Barrett2, Etana Kopin1, Jaime C Hagen1, Amy L Han1, Austin E Gillen3, Jessica Finlay-Schultz4, Diana M Cittelly4, Philip Owens4,5, Kathryn B Horwitz4,6, Carol A Sartorius3, Kirk Hansen2, Peter Kabos1.
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.Entities:
Keywords: Breast cancer; Oncology
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Year: 2020 PMID: 32045383 PMCID: PMC7101155 DOI: 10.1172/jci.insight.130751
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708