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BML-111 inhibits EMT, migration and metastasis of TAMs-stimulated triple-negative breast cancer cells via ILK pathway

Int Immunopharmacol. 2020-05-01; 
Lan Lin, Xuliang Luo, Lin Wang, Fen Xu, Yuanqiao He, Qingyu Wang, Chunlei Yuan, Jing Xu, Liping Yan, Hua Hao
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Catalog Antibody … IL-8 (DF6998) were purchased from Affinity(USA). PMA was from Sigma Aldrich (USA). BOC-2 was from GenScript Corporation (USA). The cell culture medium was from Gibco (Australia). Fetal bovine serum (FBS) was from Gibco BRL (Switzerland) … Get A Quote

摘要

Triple-negative breast cancer (TNBC) has a more aggressive phenotype and higher metastasis and recurrence rates than other breast cancer subtypes. The immune microenvironment and hypoxic microenvironment of breast cancer constitute the survival environment of cancer cells, which is an important environment to support cancer cells. LXA and its analog, BML-111 is an important regulator of inflammatory cytokines, which provides a possible way for the treatment of inflammatory-related tumors. Here, in the in vitro experiment, we showed that BML-111 could inhibit the EMT and migration of TAMs-stimulated TNBC by down-regulating ILK as well as p-Akt and p-GSK3β. And it could prevent the formation of breast cancer cel... More

關鍵詞

BML-111, ILK, Migration, TAMs, TNBC
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