Pathogenic germline variants in a racially diverse real-world cohort of prostate cancer patients

  1. Taylor B Crawford
  2. Maliha Tayeb
  3. Emanuel Barrett
  4. Tara Al-Saleem
  5. Pranavi Kondam
  6. Ryan Hausler
  7. Heather Symecko
  8. Caitlin Orr
  9. Catherine Wolfe
  10. Derek Mann
  11. Kelsey Spielman
  12. Gloria Wong
  13. Naomi Haas
  14. Vivek Narayan
  15. Kyle Robinson
  16. Samuel Takvorian
  17. Yu-Ning Wong
  18. Alexandra Sokolova
  19. Robert B. Montgomery
  20. Carolyn Menendez
  21. Michael J. Kelley
  22. Lisa B. Aiello
  23. Isla P. Garraway
  24. Susan M. Domchek
  25. Kara N. Maxwell
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Abstract

Importance

Pathogenic germline variant (PGV) rates in cancer risk genes and their association with clinical pathological features inform genetic testing practices for prostate cancer (PCa) patients.

Objective

To determine the rate of PCa risk gene PGVs in a real-world, diverse cohort of PCa patients and identify clinical predictors of carrier status.

Design, Setting, Participants, Main Outcomes and Measures

Genetic testing results for 12 PCa risk genes, clinical, pathological, and family history of cancer variables were abstracted from clinical records for 1032 PCa patients who met National Comprehensive Cancer Network (NCCN) genetic testing criteria in oncology clinics and 3602 PCa patients who underwent testing in the VA National Precision Oncology Program (VA-NPOP). Individual gene PGV rates in PCa patients were compared to cancer-free males. Statistical testing was performed by unpaired t-tests and Fisher’s exact tests, corrected for multiple testing.

Results

Of 4634 PCa patients, 5.4% had PGVs in one of 12 PCa risk genes. PGVs in BRCA2 (1.7%), ATM (1.3%), CHEK2 (1.1%), Lynch genes (0.9%), and BRCA1 (0.5%) were most common. The total PGV rate was significantly higher in 2825 self-identified White versus 1527 self-identified Black PCa patients (6.3% vs 3.7%, adjp=0.0024), although rates of BRCA2 and BRCA1 PGVs were similar (1.9% vs 1.3%, adjp=0.0885 and 0.6% vs 0.5%, adjp=0.8005, respectively). PGV rates were not significantly different in 311 Hispanic compared to 4188 non-Hispanic PCa patients (3.9% vs 5.5%, adjp=1.000). In self-identified White patients, PGV rates in ATM , BRCA1 , BRCA2, CHEK2 and Lynch genes were significantly higher compared to two cancer-free male cohorts. BRCA2 and Lynch genes PGV rates were significantly higher in PCa patients compared to a cancer-free control cohort in SIRE-Black men. In a multivariable logistic regression, age at initial PCa diagnosis and self-identified race were significantly associated with any PGV.

Conclusions and Relevance

In a racially diverse, real-world cohort of individuals with PCa, lower PGV rates were identified compared to prior academic cohort studies. Outside of ATM and CHEK2 , PGV rates were similar across the majority of clinical and pathological groupings. Our data support NCCN guideline indicated universal genetic testing for patients with aggressive forms of PCa.

Key Points

Question

What is the rate of pathogenic germline variants (PGVs) in a racially diverse, real-world cohort of prostate cancer patients who meet NCCN prostate cancer genetic testing criteria?

Findings

In this cohort study of 4634 prostate cancer patients who underwent genetic testing, we report a 5.4% PGV rate, lower than previously reported. No significant difference was seen in high-risk gene PGV rates by self-identified race or ethnicity. Age at initial PCa diagnosis, self-identified race, and prostate cancer in a first degree relative is significantly associated with having a PGV.

Meaning

Our data support current genetic testing guidelines of all patients with aggressive forms of prostate cancer.

Article activity feed

  1. Version published to 10.1101/2025.08.13.25333614 on medRxiv