Research Papers:
Whole exome sequencing in 75 high-risk families with validation and replication in independent case-control studies identifies TANGO2, OR5H14, and CHAD as new prostate cancer susceptibility genes
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Abstract
Danielle M. Karyadi1, Milan S. Geybels2, Eric Karlins1,3, Brennan Decker1, Laura McIntosh2, Amy Hutchinson3, Suzanne Kolb2, Shannon K. McDonnell4, Belynda Hicks3, Sumit Middha4, Liesel M. FitzGerald5, Melissa S. DeRycke6, Meredith Yeager3, Daniel J. Schaid4, Stephen J. Chanock3, Stephen N. Thibodeau6, Sonja I. Berndt3, Janet L. Stanford2,7,*, Elaine A. Ostrander1,*
1National Human Genome Research Institute, National Institutes of Health, Bethesda, MD, USA
2Division of Public Health Sciences, Fred Hutchinson Cancer Research Center, Seattle, WA, USA
3Division of Cancer Epidemiology and Genetics, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA
4Department of Health Sciences Research, Mayo Clinic, Rochester, MN, USA
5Menzies Institute for Medical Research, University of Tasmania, Hobart, Australia
6Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, MN, USA
7Department of Epidemiology, School of Public Health, University of Washington, Seattle, WA, USA
*Co-senior authors.
Correspondence to:
Elaine A. Ostrander, email: [email protected]
Keywords: whole exome sequencing, cancer susceptibility, high-risk families, case-control association, prostate cancer
Received: September 20, 2016 Accepted: November 07, 2016 Published: November 26, 2016
ABSTRACT
Prostate cancer (PCa) susceptibility is defined by a continuum from rare, high-penetrance to common, low-penetrance alleles. Research to date has concentrated on identification of variants at the ends of that continuum. Taking an alternate approach, we focused on the important but elusive class of low-frequency, moderately penetrant variants by performing disease model-based variant filtering of whole exome sequence data from 75 hereditary PCa families. Analysis of 341 candidate risk variants identified nine variants significantly associated with increased PCa risk in a population-based, case-control study of 2,495 men. In an independent nested case-control study of 7,121 men, there was risk association evidence for TANGO2 p.Ser17Ter and the established HOXB13 p.Gly84Glu variant. Meta-analysis combining the case-control studies identified two additional variants suggestively associated with risk, OR5H14 p.Met59Val and CHAD p.Ala342Asp. The TANGO2 and HOXB13 variants co-occurred in cases more often than expected by chance and never in controls. Finally, TANGO2 p.Ser17Ter was associated with aggressive disease in both case-control studies separately. Our analyses identified three new PCa susceptibility alleles in the TANGO2, OR5H14 and CHAD genes that not only segregate in multiple high-risk families but are also of importance in altering disease risk for men from the general population. This is the first successful study to utilize sequencing in high-risk families for the express purpose of identifying low-frequency, moderately penetrant PCa risk mutations.
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