The BMP4-BMPR1A axis represses BRCA1, inducing BRCAness in mammary stem cells and contributing to tumor initiation in basal-like breast cancer

Basal-like breast cancer (BLBC) is an aggressive subtype frequently characterized by homologous recombination deficiency (HRD) and BRCAness, even in the absence of BRCA1 mutations. Here, we identify the BMP4-BMPR1A signaling axis as a novel regulator of BRCA1 expression and a driver of BRCAness in non-transformed immature mammary cells. Analyses of patient samples reveal that high BMPR1A expression correlates with low BRCA1 levels and poor prognosis in BLBC. We show that BMP4 exposure induces BRCA1 transcriptional repression via BMPR1A, promoting a basal differentiation and impairing homologous recombination. This results in increased sensitivity to PARP inhibitors (PARPi) and accumulation of genetically unstable, immature cells. In addition, long-term BMP4 stimulation or BMPR1A overexpression induces transformation. Our findings uncover a mechanism by which the tumor microenvironment could contributes to BLBC initiation through BMP4-induced suppression of BRCA1, and suggest BMP signaling and the resultant BRCAness as a therapeutic vulnerability in BRCA1 wild-type BLBCs.