Preclinical evaluation of a novel antibody-drug conjugate OBI-992 for Cancer therapy

  • Sci Rep. 2025 Mar 13;15(1):8735. doi: 10.1038/s41598-025-92697-z.
Ting-Yu Chang  1 Chun-Jung Lin  1 Shih-Ni Wen  1 Yi-Chen Wu  1 Cheng-Yen Wei  1 Jye-Yu Huang  1 Yu-Hsuan Tsao  1 Yu-Jung Chen  1 Wei-Chien Tang  1 Yuen-Chin Wu  1 Wei-Han Lee  1 Teng-Yi Huang  1 Tzer-Min Kuo  1 Wan-Fen Li  1 Ming-Tain Lai  2
Affiliations
  • 1. OBI Pharma, Inc., 6F, No. 508, Section 7 Zhongxiao East Road, Nangang District, Taipei, Taiwan.
  • 2. OBI Pharma, Inc., 6F, No. 508, Section 7 Zhongxiao East Road, Nangang District, Taipei, Taiwan. [email protected].
Abstract

Trophoblast cell surface antigen 2 (TROP2), a Transmembrane Glycoprotein highly expressed in a variety of epithelial cancers, has been considered as a primary therapeutic target for the development of antibody-drug conjugates (ADCs). OBI-992, an investigational TROP2-targeted ADC, is composed of a novel TROP2 antibody (R4702) conjugated to the Topoisomerase I (TOP1) inhibitor exatecan through a hydrophilic enzyme-cleavable linker. This study aimed to characterize R4702 and OBI-992 in vitro. TROP2-targeted antibodies sacituzumab and datopotamab were employed as the comparators for R4702. ADCs sacituzumab govitecan (SG) and datopotamab deruxtecan (Dato-DXd) were used as benchmarks for OBI-992. Results revealed that R4702 binds to an epitope that is distinct from sacituzumab and datopotamab. The cytotoxicity of the OBI-992, SG, and Dato-DXd against different Cancer cells is comparable despite they have different internalization profile. Upregulation of breast Cancer resistance protein (BCRP) was observed in SG-resistant and Dato-DXd-resistant cells, but not in OBI-992-resistant cells. In addition, significant downregulation of TROP2 expression was detected with Dato-DXd-resistant cells and only slightly downregulation with SG- and OBI-992-resistant cells was observed. Moreover, substantial enhancement of cytotoxicity and DNA damage was found in the combination of OBI-992 with a poly (ADP-ribose) polymerase (PARP) inhibitor (talazoparib). Taken together, the findings in this study support further clinical development of OBI-992.

Keywords
Antibody–drug conjugate; Exatecan; OBI-992; TROP2; Topoisomerase I inhibitors.
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