4.7 Article

CUB Domain-Containing Protein 1 (CDCP1) Is a Target for Radioligand Therapy in Castration-Resistant Prostate Cancer, including PSMA Null Disease

CLINICAL CANCER RESEARCH (2022)

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Journal

CLINICAL CANCER RESEARCH
Volume 28, Issue 14, Pages 3066-3075

Publisher

AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1078-0432.CCR-21-3858

Keywords

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Categories

Oncology

Funding

  1. National Institutes of Health [S10RR023051, S10OD012301]
  2. Stand Up To Cancer-Prostate Cancer Foundation-Prostate Dream Team Translational Cancer Research Grant
  3. Movember Foundation
  4. NCI [1P41CA196276, CA191018]
  5. NIH [GM097316]
  6. Bristol Meyer Squibb
  7. NIH
  8. Prostate Cancer Foundation Young Investigator Award
  9. Department of Defense Prostate Cancer Research Program [W81XWH2010136]
  10. Congressionally Directed Medical Research Programs [W81XWH-21-1-0498]
  11. American Cancer Society [130635-RSG-17-005-01CCE]
  12. Precision Imaging of Cancer and Therapy program at UCSF
  13. U.S. Department of Defense (DOD) [W81XWH2010136] Funding Source: U.S. Department of Defense (DOD)

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This study found that CDCP1 is expressed in the majority of mCRPC biopsy samples, including those with low PSMA expression. Radioligand therapy targeting CDCP1 with an antibody was effective in suppressing tumor growth. These findings suggest that CDCP1 may be a potential therapeutic target for treating mCRPC.
Purpose: With the improvement in overall survival with 177Lu-PSMA 617, radioligand therapy (RLT) is now a viable option for patients with metastatic castration-resistant prostate cancer (mCRPC). However, responses are variable, in part due to low PSMA expression in 30% of patients. Herein, we evaluated whether the cell surface protein CUB domain-containing protein 1 (CDCP1) can be exploited to treat mCRPC with RLT, including in PSMA-low subsets. Experimental Design: CDCP1 levels were evaluated using RNA sequencing from 119 mCRPC biopsies. CDCP1 levels were assessed in 17 post-enzalutamide- or abiraterone-treated mCRPC biopsies, 12 patient-derived xenografts (PDX), and prostate cancer cell lines. 4A06, a recombinant human antibody that targets the CDCP1 ectodomain, was labeled with Zr-89 or Lu-177 and tested in tumor-bearing mice. Results: CDCP1 expression was observed in 90% of mCRPC biopsies, including small-cell neuroendocrine (SCNC) and adenocarcinomas with low FOLH1 (PSMA) levels. Fifteen of 17 evaluable mCRPC biopsies (85%) demonstrated membranous CDCP1 expression, and 4 of 17 (23%) had higher CDCP1 H-scores compared with PSMA. CDCP1 was expressed in 10 of 12 PDX samples. B-max values of approximately 22,000, 6,200, and 2,800 fmol/mg were calculated for PC3, DU145, and C4-2B human prostate cancer cells, respectively. Zr-89-4A06 PET detected six human prostate cancer xenografts, including PSMA-low tumors. In Lu-177-4A06 significantly suppressed growth of DU145 and C4-2B xenografts. Conclusions: The data provide the first evidence supporting CDCP1-directed RLT to treat mCRPC. Expanded studies are warranted to determine whether CDCP1 is a viable drug target for patients with mCPRC.

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