| Literature DB >> 27940127 |
Chun-Wun Lu1, Yi-Hsuan Lo1, Chu-Huang Chen2, Ching-Yi Lin1, Chun-Hao Tsai3, Po-Jung Chen1, Yi-Fang Yang1, Chie-Hong Wang1, Chun-Hsiang Tan4, Ming-Feng Hou5, Shyng-Shiou F Yuan6.
Abstract
Abnormal lipoprotein profiles are associated with breast cancer progression. However, the mechanisms linking abnormal lipoprotein levels to breast cancer progression, especially metastasis, remain unclear. Herein, we found that L1 and L5 subfractions of LDL and VLDL, but not HDL, enhanced breast cancer cell viability. L1, L5, and VLDL also increased the in vitro tumorigenesis of breast cancer cells in anchorage-independent soft agar assay. In addition, L1, L5, and VLDL, but not HDL, increased the levels of mesenchymal markers Slug, Vimentin, and β-Catenin, and promoted breast cancer cell migration and invasion. L1, L5, and VLDL increased Akt Ser473 phosphorylation and promoted cell migration, which were reversed by the PI3K/Akt inhibitor wortmannin. Further in vitro angiogenesis assay and cytokine array analysis demonstrated that L1, L5, and VLDL enhanced secretion of angiogenic factors in breast cancer cells and promoted angiogenic activity. However, only VLDL reduced anchorage-dependent cell death and promoted lung metastasis in nude mice. In summary, our data suggest that L1, L5, and especially VLDL promote breast cancer progression and metastasis through Akt-induced EMT and angiogenesis, and provide a novel mechanism of how dyslipoproteinemia promotes breast cancer progression.Entities:
Keywords: Breast cancer; LDL; Lipoprotein; Metastasis; VLDL
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Year: 2016 PMID: 27940127 DOI: 10.1016/j.canlet.2016.11.033
Source DB: PubMed Journal: Cancer Lett ISSN: 0304-3835 Impact factor: 8.679