Early cancer diagnoses through BRCA1/2 screening of unselected adult biobank participants : Genetics in Medicine : Springer Nature

Early cancer diagnoses through BRCA1/2 screening of unselected adult biobank participants : Genetics in Medicine : Springer Nature

Early cancer diagnoses through BRCA1/2screening of unselected adult biobank participants

• Adam H Buchanan MS, MPH,
• Kandamurugu Manickam MD, MPH,
• Michelle N Meyer PhD, JD,
• Jennifer K Wagner JD, PhD,
• Miranda L G Hallquist MSc,
• Janet L Williams MS,
• Alanna Kulchak Rahm PhD, MS,
• Marc S Williams MD,
• Zong-Ming E Chen MD, PhD,
• Chaitali K ShahMD,
• Tullika K Garg MD, MPH,
• Amanda L Lazzeri BS,
• Marci L B Schwartz ScM,
• D'Andra M Lindbuchler MSN,
• Audrey L Fan MS,
• Rosemary Leeming MD, MHCM,
• Pedro O Servano IIIMD,
• Ashlee L Smith DO,
• Victor G Vogel MD, MHS,
• Noura S Abul-Husn MD, PhD,
• Frederick E Dewey MD,
• Matthew S Lebo PhD,
• Heather M Mason-Suares PhD,
• Marylyn D Ritchie PhD,
• F Daniel Davis PhD
• et al.

• Affiliations
• Corresponding author

Genetics in Medicine

 

(2017)

 

doi:10.1038/gim.2017.145

Received

 

10 February 2017 

Accepted

 

12 July 2017 

Published online 

26 October 2017

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Abstract

• Abstract• 
• Introduction• 
• Materials and methods• 
• Results• 
• Discussion• 
• References• 
• Acknowledgments•
• Author information• 
• Supplementary information

Purpose

The clinical utility of screening unselected individuals for pathogenic BRCA1/2 variants has not been established. Data on cancer risk management behaviors and diagnoses of BRCA1/2-associated cancers can help inform assessments of clinical utility.

Methods

Whole-exome sequences of participants in the MyCode Community Health Initiative were reviewed for pathogenic/likely pathogenic BRCA1/2 variants. Clinically confirmed variants were disclosed to patient–participants and their clinicians. We queried patient–participants’ electronic health records for BRCA1/2-associated cancer diagnoses and risk management that occurred within 12 months after results disclosure, and calculated the percentage of patient–participants of eligible age who had begun risk management.

Results

Thirty-seven MyCode patient–participants were unaware of their pathogenic/likely pathogenic BRCA1/2 variant, had not had a BRCA1/2-associated cancer, and had 12 months of follow-up. Of the 33 who were of an age to begin BRCA1/2-associated risk management, 26 (79%) had performed at least one such procedure. Three were diagnosed with an early-stage, BRCA1/2-associated cancer—including a stage 1C fallopian tube cancer—via these procedures.

Conclusion

Screening for pathogenic BRCA1/2 variants among unselected individuals can lead to occult cancer detection shortly after disclosure. Comprehensive outcomes data generated within our learning healthcare system will aid in determining whether population-wide BRCA1/2 genomic screening programs offer clinical utility.

Keywords:

BRCA1; BRCA2; biobank; Hereditary Breast and Ovarian Cancer Syndrome; Whole Exome sequencing