Siglec15/TGF- bispecific antibody mediates synergistic anti-tumor response against 4T1 triple negative breast cancer in mice

An ideal tumor-specific immunomodulatory therapy should both preferentially target the tumor, while simultaneously reduce the immunosuppressive environment within the tumor. This guiding principle led us to explore engineering Siglec-15 (S15) targeted bispecific antibody (bsAb) to enhance therapy against triple negative breast cancer (TNBC). S15 appears to be exclusively expressed on macrophages and diverse tumor cells, including human and mouse 4T1 TNBC. TGF-beta is a growth hormone frequently associated with increased tumor invasiveness, including in TNBC. Here, to overcome the immune-suppressive environment within TNBC tumors to enable more effective cancer therapy, we engineered a bispecific antibody (bsAb) targeting both Siglec15 and TGF-beta. In mice engrafted with orthotopic 4T1 tumors, S15/TGF-beta bsAb treatment was highly effective in suppressing tumor growth, not only compared to control monoclonal antibody (mAb) but also markedly more effective than mAbs against S15 alone, against TGF-beta alone, as well as a cocktail of both anti-S15 and anti-TGF-beta mAbs. We did not detect liver and lung metastasis in mice treated with S15/TGF-beta bsAb, unlike all other treatment groups at the end of the study. The enhanced anti-tumor response observed with S15/TGF-beta bsAb correlated with a less immunosuppressive environment in the tumor. These results underscore S15-targeted bsAb as a promising therapeutic strategy for TNBC, and possibly other S15 positive solid tumors.