Upregulated WAVE3 expression is essential for TGF-β-mediated EMT and metastasis of triple-negative breast cancer cells.

[wiskott-aldrich syndrome]

Breast cancer is the second leading cause of cancer death in women in the United States . Metastasis accounts for the death of ~90 % of these patients , yet the mechanisms underlying this event remain poorly defined . WAVE 3 belongs to the WASP /WAVE family of actin-binding proteins that play essential roles in regulating cell morphology , actin polymerization , cytoskeleton remodeling , cell motility , and invasion . Accordingly , we demonstrated previously that WAVE 3 promotes the acquisition of invasive and metastatic phenotypes by human breast cancers . Herein , we show that transforming growth factor -β (TGF-β ) selectively and robustly induced the expression of WAVE 3 in metastatic breast cancer cells , but not in their nonmetastatic counterparts . Moreover , the induction of WAVE 3 expression in human and mouse triple-negative breast cancer cells (TNBCs ) by TGF-β likely reflects its coupling to microRNA expression via a Smad 2 - and β 3 integrin-dependent mechanism . We further demonstrate the requirement for WAVE 3 expression in mediating the initiation of epithelial-mesenchymal transition (EMT ) programs stimulated by TGF-β . Indeed , stable depletion of WAVE 3 expression in human TNBC cells prevented TGF-β from inducing EMT programs and from stimulating the proliferation , migration , and the formation of lamellipodia in metastatic TNBC cells . Lastly , we observed WAVE 3 deficiency to abrogate the outgrowth of TNBC cell organoids in 3 -dimensional organotypic cultures as well as to decrease the growth and metastasis of 4 T 1 tumors produced in syngeneic Balb /C mice . Indeed , WAVE 3 deficiency significantly reduced the presence of sarcomatoid morphologies indicative of EMT phenotypes in pulmonary TNBC tumors as compared to those detected in their parental counterparts . Collectively , these findings indicate the necessity for WAVE 3 expression and activity during EMT programs stimulated by TGF-β ; they also suggest that measures capable of inactivating WAVE 3 may play a role in alleviating metastasis stimulated by TGF-β .