Inherited TP53 variants and risk of prostate cancer Journal Article

   


Authors: Maxwell, K. N.; Cheng, H. H.; Powers, J.; Gulati, R.; Ledet, E. M.; Morrison, C.; Le, A.; Hausler, R.; Stopfer, J.; Hyman, S.; Kohlmann, W.; Naumer, A.; Vagher, J.; Greenberg, S. E.; Naylor, L.; Laurino, M.; Konnick, E. Q.; Shirts, B. H.; AlDubayan, S. H.; Van Allen, E. M.; Nguyen, B.; Vijai, J.; Abida, W.; Carlo, M. I.; Dubard-Gault, M.; Lee, D. J.; Maese, L. D.; Mandelker, D.; Montgomery, B.; Morris, M. J.; Nicolosi, P.; Nussbaum, R. L.; Schwartz, L. E.; Stadler, Z.; Garber, J. E.; Offit, K.; Schiffman, J. D.; Nelson, P. S.; Sartor, O.; Walsh, M. F.; Pritchard, C. C.
Article Title: Inherited TP53 variants and risk of prostate cancer
Abstract: Background: Inherited germline TP53 pathogenic and likely pathogenic variants (gTP53) cause autosomal dominant multicancer predisposition including Li-Fraumeni syndrome (LFS). However, there is no known association of prostate cancer with gTP53. Objective: To determine whether gTP53 predisposes to prostate cancer. Design, setting, and participants: This multi-institutional retrospective study characterizes prostate cancer incidence in a cohort of LFS males and gTP53 prevalence in a prostate cancer cohort. Outcome measurements and statistical analysis: We evaluated the spectrum of gTP53 variants and clinical features associated with prostate cancer. Results and limitations: We identified 31 prostate cancer cases among 163 adult LFS males, including 26 of 54 aged ≥50 yr. Among 117 LFS males without prostate cancer at the time of genetic testing, six were diagnosed with prostate cancer over a median (interquartile range [IQR]) of 3.0 (1.3–7.2) yr of follow-up, a 25-fold increased risk (95% confidence interval [CI] 9.2–55; p < 0.0001). We identified gTP53 in 38 of 6850 males (0.6%) in the prostate cancer cohort, a relative risk 9.1-fold higher than that of population controls (95% CI 6.2–14; p < 0.0001; gnomAD). We observed hotspots at the sites of attenuated variants not associated with classic LFS. Two-thirds of available gTP53 prostate tumors had somatic inactivation of the second TP53 allele. Among gTP53 prostate cancer cases in this study, the median age at diagnosis was 56 (IQR: 51–62) yr, 44% had Gleason ≥8 tumors, and 29% had advanced disease at diagnosis. Conclusions: Complementary analyses of prostate cancer incidence in LFS males and gTP53 prevalence in prostate cancer cohorts suggest that gTP53 predisposes to aggressive prostate cancer. Prostate cancer should be considered as part of LFS screening protocols and TP53 considered in germline prostate cancer susceptibility testing. Patient summary: Inherited pathogenic variants in the TP53 gene are likely to predispose men to aggressive prostate cancer. © 2021 The Author(s)
Keywords: adult; controlled study; human tissue; aged; middle aged; young adult; gene mutation; major clinical study; clinical feature; cancer risk; follow up; cancer diagnosis; cancer incidence; allele; germline; cancer susceptibility; incidence; prevalence; cohort analysis; genetic variability; retrospective study; protein p53; carcinogenesis; prostate cancer; gleason score; screening; li-fraumeni syndrome; genetic screening; genetic testing; tp53; very elderly; human; male; article; hypomorphic mutation; pathogenic variant; attenuated; inherited cancer syndrome
Journal Title: European Urology
Volume: 81
Issue: 3
ISSN: 0302-2838
Publisher: Elsevier Science, Inc.  
Date Published: 2022-03-01
Start Page: 243
End Page: 250
Language: English
DOI: 10.1016/j.eururo.2021.10.036
PUBMED: 34863587
PROVIDER: scopus
PMCID: PMC8891030
DOI/URL:

https://www.scopus.com/inward/record.uri?eid=2-s2.0-85120477352&doi=10.1016%2fj.eururo.2021.10.036&partnerID=40&md5=1924a5090d262adf1d82f111d535bbcd
Notes: Article -- Funding details: Abramson Cancer Center, ACC, P30CA008748 -- Vijai Joseph's first and last names are reversed on the original publication -- Source: Scopus
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MSK Authors
  1. Kenneth Offit
    788 Offit
  2. Michael Morris
    577 Morris
  3. Zsofia Kinga Stadler
    387 Stadler
  4. Vijai Joseph
    211 Joseph
  5. Wassim Abida
    154 Abida
  6. Maria Isabel Carlo
    161 Carlo
  7. Michael Francis Walsh
    156 Walsh
  8. Diana Lauren Mandelker
    178 Mandelker
  9. Bastien Nguyen
    31 Nguyen
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