Genetic Risk for Subsequent Neoplasms Among Long-Term Survivors of Childhood Cancer

Zhaoming Wang(St. Jude Children's Research Hospital), Carmen L. Wilson(St. Jude Children's Research Hospital), John Easton(St. Jude Children's Research Hospital), Andrew Thrasher(St. Jude Children's Research Hospital), Heather L. Mulder(St. Jude Children's Research Hospital), Qi Liu(St. Jude Children's Research Hospital), Dale J. Hedges(St. Jude Children's Research Hospital), Shuoguo Wang(St. Jude Children's Research Hospital), Michael Rusch(St. Jude Children's Research Hospital), Michael N. Edmonson(St. Jude Children's Research Hospital), Shawn Levy(St. Jude Children's Research Hospital), Jennifer Q. Lanctot(St. Jude Children's Research Hospital), Eric Caron(St. Jude Children's Research Hospital), Kyla Shelton(St. Jude Children's Research Hospital), Kelsey Currie(St. Jude Children's Research Hospital), Matthew Lear(St. Jude Children's Research Hospital), Aman Patel(St. Jude Children's Research Hospital), Celeste Rosencrance(St. Jude Children's Research Hospital), Ying Shao(St. Jude Children's Research Hospital), Bhavin Vadodaria(St. Jude Children's Research Hospital), Donald Yergeau(St. Jude Children's Research Hospital), Yadav Sapkota(St. Jude Children's Research Hospital), Russell J. Brooke(St. Jude Children's Research Hospital), Wonjong Moon(St. Jude Children's Research Hospital), Evadnie Rampersaud(St. Jude Children's Research Hospital), Xiaotu Ma(St. Jude Children's Research Hospital), Ti-Cheng Chang(St. Jude Children's Research Hospital), Stephen V. Rice(St. Jude Children's Research Hospital), Cynthia Pepper(St. Jude Children's Research Hospital), Xin Zhou(St. Jude Children's Research Hospital), Xiang Chen(St. Jude Children's Research Hospital), Wenan Chen(St. Jude Children's Research Hospital), Angela Jones(St. Jude Children's Research Hospital), Braden Boone(St. Jude Children's Research Hospital), Matthew J. Ehrhardt(St. Jude Children's Research Hospital), Matthew J. Krasin(St. Jude Children's Research Hospital), Rebecca M. Howell(St. Jude Children's Research Hospital), Nicholas S. Phillips(St. Jude Children's Research Hospital), Courtney Lewis(St. Jude Children's Research Hospital), Deo Kumar Srivastava(St. Jude Children's Research Hospital), Ching‐Hon Pui(St. Jude Children's Research Hospital), Chimene Kesserwan(St. Jude Children's Research Hospital), Gang Wu(St. Jude Children's Research Hospital), Kim E. Nichols(St. Jude Children's Research Hospital), James R. Downing(St. Jude Children's Research Hospital), Melissa M. Hudson(St. Jude Children's Research Hospital), Yutaka Yasui(St. Jude Children's Research Hospital), Leslie L. Robison(St. Jude Children's Research Hospital), Jinghui Zhang(St. Jude Children's Research Hospital)
Journal of Clinical Oncology
May 30, 2018
10.1200/jco.2018.77.8589
Cited by 144Open Access
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Abstract

Purpose Childhood cancer survivors are at increased risk of subsequent neoplasms (SNs), but the germline genetic contribution is largely unknown. We assessed the contribution of pathogenic/likely pathogenic (P/LP) mutations in cancer predisposition genes to their SN risk. Patients and Methods Whole-genome sequencing (30-fold) was performed on samples from childhood cancer survivors who were ≥ 5 years since initial cancer diagnosis and participants in the St Jude Lifetime Cohort Study, a retrospective hospital-based study with prospective clinical follow-up. Germline mutations in 60 genes known to be associated with autosomal dominant cancer predisposition syndromes with moderate to high penetrance were classified by their pathogenicity according to the American College of Medical Genetics and Genomics guidelines. Relative rates (RRs) and 95% CIs of SN occurrence by mutation status were estimated using multivariable piecewise exponential regression stratified by radiation exposure. Results Participants were 3,006 survivors (53% male; median age, 35.8 years [range, 7.1 to 69.8 years]; 56% received radiotherapy), 1,120 SNs were diagnosed among 439 survivors (14.6%), and 175 P/LP mutations were identified in 5.8% (95% CI, 5.0% to 6.7%) of survivors. Mutations were associated with significantly increased rates of breast cancer (RR, 13.9; 95% CI, 6.0 to 32.2) and sarcoma (RR, 10.6; 95% CI, 4.3 to 26.3) among irradiated survivors and with increased rates of developing any SN (RR, 4.7; 95% CI, 2.4 to 9.3), breast cancer (RR, 7.7; 95% CI, 2.4 to 24.4), nonmelanoma skin cancer (RR, 11.0; 95% CI, 2.9 to 41.4), and two or more histologically distinct SNs (RR, 18.6; 95% CI, 3.5 to 99.3) among nonirradiated survivors. Conclusion The findings support referral of all survivors for genetic counseling for potential clinical genetic testing, which should be prioritized for nonirradiated survivors with any SN and for those with breast cancer or sarcoma in the field of prior irradiation.

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