AI Article Synopsis
- Metastasis is a major cause of cancer-related deaths, with specific interactions between tumor cells and their surrounding environment playing a critical role in this process.
- The transcription factor c-Myb is linked to breast cancer progression; however, this study reveals that higher c-Myb levels actually inhibit lung metastasis by disrupting the ability of tumor cells to exit blood vessels.
- Cells with lower c-Myb levels show increased metastatic potential and are associated with an inflammatory signature dominated by Ccl2, indicating that c-Myb may help reduce inflammation and prevent lung metastasis in breast cancer patients.
Article Abstract
Metastasis accounts for most of cancer-related deaths. Paracrine signaling between tumor cells and the stroma induces changes in the tumor microenvironment required for metastasis. Transcription factor c-Myb was associated with breast cancer (BC) progression but its role in metastasis remains unclear. Here we show that increased c-Myb expression in BC cells inhibits spontaneous lung metastasis through impaired tumor cell extravasation. On contrary, BC cells with increased lung metastatic capacity exhibited low c-Myb levels. We identified a specific inflammatory signature, including Ccl2 chemokine, that was expressed in lung metastatic cells but was suppressed in tumor cells with higher c-Myb levels. Tumor cell-derived Ccl2 expression facilitated lung metastasis and rescued trans-endothelial migration of c-Myb overexpressing cells. Clinical data show that the identified inflammatory signature, together with a MYB expression, predicts lung metastasis relapse in BC patients. These results demonstrate that the c-Myb-regulated transcriptional program in BCs results in a blunted inflammatory response and consequently suppresses lung metastasis.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6711763 | PMC |
| http://dx.doi.org/10.1038/onc.2017.392 | DOI Listing |
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