mAbs (Dec 2024)

Discovery of a novel highly specific, fully human PSCA antibody and its application as an antibody-drug conjugate in prostate cancer

  • Xiaojie Chu,
  • Seungmin Shin,
  • Du-San Baek,
  • Liyong Zhang,
  • Alex Conard,
  • Megan Shi,
  • Ye-Jin Kim,
  • Cynthia Adams,
  • Maggie Hines,
  • Xianglei Liu,
  • Chuan Chen,
  • Zehua Sun,
  • Dontcho V. Jelev,
  • John W. Mellors,
  • Dimiter S. Dimitrov,
  • Wei Li

DOI
https://doi.org/10.1080/19420862.2024.2387240
Journal volume & issue
Vol. 16, no. 1

Abstract

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Prostate stem cell antigen (PSCA) is expressed in all stages of prostate cancer, including in advanced androgen-independent tumors and bone metastasis. PSCA may associate with prostate carcinogenesis and lineage plasticity in prostate cancer. PSCA is also a promising theranostic marker for a variety of other solid tumors, including pancreatic adenocarcinoma and renal cell carcinoma. Here, we identified a novel fully human PSCA antibody using phage display methodology. The structure-based affinity maturation yielded a high-affinity binder, F12, which is highly specific and does not bind to 6,000 human membrane proteins based on a membrane proteome array assay. F12 targets PSCA amino acids 63–69 as tested by the peptide scanning microarray, and it cross-reacts with the murine PSCA. IgG1 F12 efficiently internalizes into PSCA-expressing tumor cells. The antimitotic reagent monomethyl auristatin E (MMAE)-conjugated IgG1 F12 (ADC, F12-MMAE) exhibits dose-dependent efficacy and specificity in a human prostate cancer PC-3-PSCA xenograft NSG mouse model. This is a first reported ADC based on a fully human PSCA antibody and MMAE that is characterized in a xenograft murine model, which warrants further optimizations and investigations in additional preclinical tumor models, including prostate and other solid tumors.

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