Compelling evidence for a prostate cancer gene at 22q12.3 by the International Consortium for Prostate Cancer Genetics

doi:10.1093/hmg/ddm075

Human Molecular Genetics Advance Access originally published online on May 3, 2007
Human Molecular Genetics 2007 16(11):1271-1278; doi:10.1093/hmg/ddm075

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Compelling evidence for a prostate cancer gene at 22q12.3 by the International Consortium for Prostate Cancer Genetics

Nicola J. Camp¹^,*, Lisa A. Cannon-Albright¹, James M. Farnham¹, Agnes B. Baffoe-Bonnie²^,3^,4, Asha George²^,3, Isaac Powell²^,5, Joan E. Bailey-Wilson²^,4, John D. Carpten²^,6, Graham G. Giles⁷^,8, John L. Hopper⁷^,9, Gianluca Severi⁷^,8, Dallas R. English⁷^,9, William D. Foulkes⁷^,10, Lovise Maehle⁷^,11, Pal Moller⁷^,11, Ros Eeles⁷^,12, Douglas Easton⁷^,13, Michael D. Badzioch⁷^,14, Alice S. Whittemore¹⁵^,16^,17, Ingrid Oakley-Girvan¹⁵^,17, Chih-Lin Hsieh¹⁵^,18, Latchezar Dimitrov¹⁹, Jianfeng Xu¹⁹, Janet L. Stanford²⁰^,21, Bo Johanneson²⁰^,22, Kerry Deutsch²⁰^,23, Laura McIntosh²⁰^,21, Elaine A. Ostrander²⁰^,22, Kathleen E. Wiley²⁴, Sarah D. Isaacs²⁴, Patrick C. Walsh²⁴, Stephen N. Thibodeau²⁵, Shannon K. McDonnell²⁵, Scott Hebbring²⁵, Daniel J. Schaid²⁵, Ethan M. Lange²⁶^,27, Kathleen A. Cooney²⁶^,28, Teuvo L.J. Tammela²⁹, Johanna Schleutker²⁹, Thomas Paiss³⁰^,31, Christiane Maier³⁰^,32, Henrik Grönberg³³^,35, Fredrik Wiklund³³^,35, Monica Emanuelsson³³^,34, William B. Isaacs for the International Consortium for Prostate Cancer Genetics²⁴

¹ University of Utah ICPCG Group and Division of Genetic Epidemiology, University of Utah School of Medicine, 391, Chipeta Way, Suite D, Salt Lake City, UT 84108, USA, ² African American Hereditary Prostate Cancer ICPCG Group, ³ Fox Chase Cancer Center, Philadelphia, PA, USA, ⁴ National Human Genome Research Institute, NIH, Bethesda, MD, USA, ⁵ Karmanos Cancer Institute, Wayne State University, Detroit, MI, USA, ⁶ Translational Genomics Research Institute, Genetic Basis of Human Disease Research Division, Phoenix, AZ, USA, ⁷ ACTANE Consortium ICPCG Group, ⁸ Cancer Epidemiology Centre, The Cancer Council Victoria, Melbourne, Australia, ⁹ Centre for Molecular, Environmental, Genetic and Analytic Epidemiology, School of Population Health, The University of Melbourne, Melbourne, Australia, ¹⁰ Department of Oncology, McGill University, Montreal, Quebec, Canada, ¹¹ The Norwegian Radium Hospital, Oslo, Norway, ¹² Institute of Cancer Research, Royal Marsden NHS Foundation Trust, Surrey, UK, ¹³ Cancer Research UK Genetic Epidemiology Unit, Cambridge, UK, ¹⁴ Division of Medical Genetics, University of Washington Medical Center, Seattle, WA, USA, ¹⁵ BC/CA/HI ICPCG Group, ¹⁶ Department of Health Research and Policy, ¹⁷ Stanford Comprehensive Cancer Center, Stanford School of Medicine, CA, USA, ¹⁸ Department of Urology and Department of Biochemistry and Molecular Biology, University of Southern California, CA, USA, ¹⁹ Data Coordinating Center for the ICPCG and Center for Human Genomics, Wake Forest University School of Medicine, Winston-Salem, NC, USA, ²⁰ FHCRC ICPCG Group, ²¹ Fred Hutchinson Cancer Research Center, Divisions of Public Health Sciences, Seattle, WA, USA, ²² Cancer Genetics Branch, National Institutes of Health, Bethesda, MD, USA, ²³ Institute for Systems Biology, Seattle, WA, USA, ²⁴ Johns Hopkins University ICPCG group and Department of Urology, Johns Hopkins Medical Institutions, Baltimore, MD, USA, ²⁵ Mayo Clinic ICPCG Group and Mayo Clinic, Rochester, MN, USA, ²⁶ University of Michigan ICPCG Group, ²⁷ Department of Genetics, University of North Carolina, Chapel Hill, NC, USA, ²⁸ University of Michigan, Ann Arbor, MI, USA, ²⁹ University of Tampere ICPCG group and Tampere University Hospital, University of Tampere, Tampere, Finland, ³⁰ University of Ulm ICPCG group, ³¹ Department of Urology, ³² Institute of Human Genetics, University of Ulm, Germany, ³³ University of Umeå ICPCG group, ³⁴ Oncologic Centre, Umeå University, Umeå, Sweden and ³⁵ Department of Medical Epidemiology and Biostatistics, Karolinska Institutet, Stockholm, Sweden

^* To whom correspondence should be addressed. Tel: +1 8015879351; Fax: +1 8015816052; Email: nicola.camp{at}utah.edu

Received January 28, 2007; Accepted March 20, 2007

Previously, an analysis of 14 extended, high-risk Utah pedigreeslocalized in the chromosome 22q linkage region to 3.2 Mbat 22q12.3-13.1 (flanked on each side by three recombinants)contained 31 annotated genes. In this large, multi-centered,collaborative study, we performed statistical recombinant mappingin 54 pedigrees selected to be informative for recombinant mappingfrom nine member groups of the International Consortium forProstate Cancer Genetics (ICPCG). These 54 pedigrees includedthe 14 extended pedigrees from Utah and 40 pedigrees from eightother ICPCG member groups. The additional 40 pedigrees wereselected from a total pool of 1213 such that each pedigree wasrequired to contain both at least four prostate cancer (PRCA)cases and exhibit evidence for linkage to the chromosome 22qregion. The recombinant events in these 40 independent pedigreesconfirmed the previously proposed region. Further, when all54 pedigrees were considered, the three-recombinant consensusregion was narrowed down by more than a megabase to 2.2 Mbat chromosome 22q12.3 flanked by D22S281 and D22S683. This narrowerregion eliminated 20 annotated genes from that previously proposed,leaving only 11 genes. This region at 22q12.3 is the most consistentlyidentified and smallest linkage region for PRCA. This collaborativestudy by the ICPCG illustrates the value of consortium effortsand the continued utility of linkage analysis using informativepedigrees to localize genes for complex diseases.

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