Targeting the Vav1/miR­29b axis as a potential approach for treating selected molecular subtypes of triple­negative breast cancer.

MicroRNA (miR)­29b has been reported to play a controversial role in breast cancer, particularly triple­negative breast cancer (TNBC). Based on our previous data revealing that the PU.1­mediated expression of miR­29b in cells from acute myeloid leukemia is sustained by Vav1, the potential role of this multidomain protein in modulating miR­29b levels in breast tumor cells, in which Vav1 is ecstopically expressed and shows a nuclear accumulation, was investigated. Breast cancer cell lines with various phenotypes and patient­derived xenograft­derived TNBC cells were subjected to Vav1 modulation and reverse transcription quantitative PCR of miR­29b levels. The recruitment of CCAAT enhancer binding protein α (CEBPα) to miR­29b promoters was investigated by quantitative chromatin immunoprecipitation assays. It was found that Vav1 was essential for the recovery of mature miR­29b in breast cancer cell lines, and that it promoted the expression of the miRNA in TNBC cells of the mesenchymal molecular subtype by sustaining the transcription of the miR­29b1/a cluster mediated by CEBPα. The present results suggest that Vav1 is a crucial modulator of miR­29b expression in breast tumor cells, and this finding may help identify strategies that may be useful in the management of TNBC by targeting the Vav1/miR­29b axis, as there is a lack of molecular­based treatments for TNBC.