Abstract
BackgroundProlactin receptor (PRLR) is highly expressed in a subset of human breast cancer and prostate cancer, which makes it a potential target for cancer treatment. In clinical trials, the blockade of PRLR was shown to be safe but with poor efficacy. It is therefore urgent to develop new therapies against PRLR target. Bispecific antibodies (BsAbs) could guide immune cells toward tumor cells, and produced remarkable effects in some cancers.MethodsIn this study, a bispecific antibody targeting both tumor antigen PRLR and T cell surface CD3 antigen (PRLR-DbsAb) was constructed by split intein mediated protein transsplicing (BAPTS) system for the first time. Its binding activity was determined by Biacore and Flow cytometry, and target-dependent T cell mediated cytotoxicity was detected using LDH release assay. ELISA was utilized to study the secretion of cytokines by immune cells. Subcutaneous tumor mouse models were used to analyze the in vivo anti-tumor effects of PRLR-DbsAb.ResultsPRLR-DbsAb in vitro could recruit and activate T cells to promote the release of Th1 cytokines IFN- γ and TNF- α, which could kill PRLR expressed breast cancer cells. In xenograft models with breast cancer cell line T47D, NOD/SCID mice intraperitoneally injected with PRLR-DbsAb exhibited significant inhibition of tumor growth and a longer survival compared to mice treated with PRLR monoclonal antibody (PRLR mAb).ConclusionsBoth in vitro and in vivo experiments showed PRLR-DbsAb had a potential therapy of cancer treatment potential therapy for cancer. Immunotherapy may be a promising treatment against the tumor target of PRLR.
Highlights
Prolactin receptor (PRLR) is highly expressed in a subset of human breast cancer and prostate cancer, which makes it a potential target for cancer treatment
Purified PRLR-DbsAb recruits T cells to PRLR-expression T47D cells we investigated the mechanism of killing of breast cancer cells mediated by the bispecific antibody PRLRDbsAb targeting CD3 and PRLR
Agarwal et al has reported a negative result of PRLR Monoclonal antibody (mAb) LFA102 for the treatment of metastatic PRLR positive breast cancer and metastatic castration resistant prostate cancer in phase I clinical trials (10)
Summary
Prolactin receptor (PRLR) is highly expressed in a subset of human breast cancer and prostate cancer, which makes it a potential target for cancer treatment. The blockade of PRLR was shown to be safe but with poor efficacy. PRLR is one kind of type I cytokine receptors highly expressed in breast cancer cells [1]. It is only slightly expressed in normal breast tissues while highly expressed in tumor breast tissues [1,2,3]. The blocking PRLR antibody has shown a very good safety profile in phase I clinical trials [6].
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