[No authors listed]
Tripleânegative breast cancer (TNBC) is a subtype of breast cancer with a high degree of malignancy. TNBC is prone to distant metastasis and has a poor prognosis. A number of TNBCârelated microRNAs (miRNAs) have been studied and identified. However, the detailed roles of miRâ574â5p in TNBC remain poorly understood. miRâ574â5p, SRY (sex determining region Y)âbox 2 (SOX2), Bâcell lymphoma/leukaemia 11A (BCL11A), SKI like protoâoncogene (SKIL) and epithelialâmesenchymal transition (EMT)ârelated miRNAs and proteins were measured by reverse transcriptionâquantitative PCR and western blotting analysis, respectively. A luciferase reporter assay was employed to validate the direct targeting of SOX2 and BCL11A by miRâ574â5p. MTT, colony formation and Transwell assays were performed to analyse the biological functions of miRâ574â5p in TNBC cells. A nude mouse xenograft model was used to verify the effects of miRâ574â5p on the tumorigenesis of TNBC in vivo. The results demonstrated that miRâ574â5p levels were decreased in breast cancer tissues and cells. miRâ574â5p repressed proliferation, migration and EMT in TNBC cells. Further experiments confirmed that miRâ574â5p reduced tumour size and metastasis in vivo. miRâ574â5p targeted BCL11A and SOX2 to inhibit the SKIL/transcriptional coâactivator with PDZâbinding motif/connective tissue growth factor axis, and the inhibitory effect of miRâ574â5p in TNBC cells was at least partly dependent on SOX2 and BCL11A. In addition, the regulation of downstream oncogenes by SOX2 was dependent on BCL11A. To the best of our knowledge, this is the first study to report the association between the miRâ574â5p/BCL11A/SOX2 axis and the tumorigenesis of TNBC, which provides a new mechanism for understanding the progression of TNBC.
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