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Gene-based confirmatory germline testing following tumor-only sequencing of prostate cancer

  • Hong Truong,
  • Kelsey Breen,
  • Subhiksha Nandakumar,
  • Daniel D. Sjoberg,
  • Yelena Kemel,
  • Nikita Mehta,
  • Andrew T. Lenis,
  • Peter A. Reisz,
  • Jessica Carruthers,
  • Nicole Benfante,
  • Vijai Joseph,
  • Aliya Khurram,
  • Anuradha Gopalan,
  • Samson W. Fine,
  • Victor E. Reuter,
  • Andrew J. Vickers,
  • Ozge Birsoy,
  • Ying Liu,
  • Michael Walsh,
  • Alicia Latham,
  • Diana Mandelker,
  • Zsofia K. Stadler,
  • Eugene Pietzak,
  • Behfar Ehdaie,
  • Karim A. Touijer,
  • Vincent P. Laudone,
  • Susan F. Slovin,
  • Karen A. Autio,
  • Daniel C. Danila,
  • Dana E. Rathkopf,
  • James A. Eastham,
  • Yu Chen,
  • Michael J. Morris,
  • Kenneth Offit,
  • David B. Solit,
  • Howard I. Scher,
  • Wassim Abida,
  • Mark E. Robson,
  • Maria I. Carlo

Publication: European Urology, September 2022

https://www.europeanurology.com/article/S0302-2838(22)02619-7/fulltext

Background

Tumor-only genomic profiling is an important tool in therapeutic management of men with prostate cancer. Since clinically actionable germline variants may be reflected in tumor profiling, it is critical to identify which variants have a higher risk of being germline in origin to better counsel patients and prioritize genetic testing.

Objective

To determine when variants found on tumor-only sequencing of prostate cancers should prompt confirmatory germline testing.

Design, setting, and participants

Men with prostate cancer who underwent both tumor and germline sequencing at Memorial Sloan Kettering Cancer Center from January 1, 2015 to January 31, 2020 were evaluated.

Outcome measurements and statistical analysis

Tumor and germline profiles were analyzed for pathogenic and likely pathogenic (“pathogenic”) variants in 60 moderate- or high-penetrance genes associated with cancer predisposition. The germline probability (germline/germline + somatic) of a variant was calculated for each gene. Clinical and pathologic factors were analyzed as potential modifiers of germline probability.

Results and limitations

Of the 1883 patients identified, 1084 (58%) had a somatic or germline pathogenic variant in one of 60 cancer susceptibility genes, and of them, 240 (22%) had at least one germline variant. Overall, the most frequent variants were in TP53, PTEN, APC, BRCA2, RB1, ATM, and CHEK2. Variants in TP53, PTEN, or RB1 were identified in 746 (40%) patients and were exclusively somatic. Variants with the highest germline probabilities were in PALB2 (69%), MITF (62%), HOXB13 (60%), CHEK2 (55%), BRCA1 (55%), and BRCA2 (47%), and the overall germline probability of a variant in any DNA damage repair gene was 40%. Limitations were that most of the men included in the cohort had metastatic disease, and different thresholds for pathogenicity exist for somatic and germline variants.

Conclusions

Of patients with pathogenic variants found on prostate tumor sequencing, 22% had clinically actionable germline variants, for which the germline probabilities varied widely by gene. Our results provide an evidenced-based clinical framework to prioritize referral to genetic counseling following tumor-only sequencing.