Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q

Matthew B. McQueen; B. Devlin; Stephen V. Faraone; Vishwajit L. Nimgaonkar; Pamela Sklar; Jordan W. Smoller; Rami Abou Jamra; Margot Albus; Silviu Alin Bacanu; Miron Baron; Thomas B. Barrett; Wade Berrettini; Deborah Blacker; William Byerley; Sven Cichon; Willam Coryell; Nick Craddock; Mark J. Daly; J. Raymond DePaulo; Howard J. Edenberg; Tatiana Foroud; Michael Gill; T. Conrad Gilliam; Marian Hamshere; Ian Jones; Lisa Jones; Suh Hang Juo; John R. Kelsoe; David Lambert; Christoph Lange; Bernard Lerer; Jianjun Liu; Wolfgang Maier; James D. MacKinnon; Melvin G. McInnis; Francis J. McMahon; Dennis L. Murphy; Markus M. Nöthen; John I. Nurnberger; Carlos N. Pato; Michele T. Pato; James B. Potash; Peter Propping; Ann E. Pulver; John P. Rice; Marcella Rietschel; William Scheftner; Johannes Schumacher; Ricardo Segurado; Kristel Van Steen; Weiting Xie; Peter P. Zandi; Nan M. Laird

doi:10.1086/491603

Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q

Matthew B. McQueen
, B. Devlin
, Stephen V. Faraone
, Vishwajit L. Nimgaonkar
, Pamela Sklar
, Jordan W. Smoller
, Rami Abou Jamra
, Margot Albus
, Silviu Alin Bacanu
, Miron Baron
, Thomas B. Barrett
, Wade Berrettini
, Deborah Blacker
, William Byerley
, Sven Cichon
, Willam Coryell
, Nick Craddock
, Mark J. Daly
, J. Raymond DePaulo
, Howard J. Edenberg

Tatiana Foroud, Michael Gill, T. Conrad Gilliam, Marian Hamshere, Ian Jones, Lisa Jones, Suh Hang Juo, John R. Kelsoe, David Lambert, Christoph Lange, Bernard Lerer, Jianjun Liu, Wolfgang Maier, James D. MacKinnon, Melvin G. McInnis, Francis J. McMahon, Dennis L. Murphy, Markus M. Nöthen, John I. Nurnberger, Carlos N. Pato, Michele T. Pato, James B. Potash, Peter Propping, Ann E. Pulver, John P. Rice, Marcella Rietschel, William Scheftner, Johannes Schumacher, Ricardo Segurado, Kristel Van Steen, Weiting Xie, Peter P. Zandi, Nan M. Laird

Psychiatry

Upstate Medical University

Harvard University
Massachusetts General Hospital
University of Pittsburgh
Massachusetts Institute of Technology
University of Bonn
Isar-Amper-Klinikum München-Ost
GlaxoSmithKline
Columbia University
University of California at San Diego
Department of Veterans Affairs
University of Pennsylvania
University of California at San Francisco
University of Iowa
Cardiff University
Whitehead Institute
Johns Hopkins University
Indiana University Bloomington
Trinity College Dublin
The University of Chicago
University of Birmingham
Hadassah University Medical Centre
Agency for Science, Technology and Research, Singapore
National Institutes of Health
State University of New York (SUNY)
Washington University St. Louis
Zentralinstitut fur Seelische Gesundheit
Rush University

Research output: Contribution to journal › Article › peer-review

193 Scopus citations

Abstract

Several independent studies and meta-analyses aimed at identifying genomic regions linked to bipolar disorder (BP) have failed to find clear and consistent evidence of linkage regions. Our hypothesis is that combining the original genotype data provides benefits of increased power and control over sources of heterogeneity that outweigh the difficulty and potential pitfalls of the implementation. We conducted a combined analysis using the original genotype data from 11 BP genomewide linkage scans comprising 5,179 individuals from 1,067 families. Heterogeneity among studies was minimized in our analyses by using uniform methods of analysis and a common, standardized marker map and was assessed using novel methods developed for meta-analysis of genome scans. To date, this collaboration is the largest and most comprehensive analysis of linkage samples involving a psychiatric disorder. We demonstrate that combining original genome-scan data is a powerful approach for the elucidation of linkage regions underlying complex disease. Our results establish genomewide significant linkage to BP on chromosomes 6q and 8q, which provides solid information to guide future gene-finding efforts that rely on fine-mapping and association approaches.

Original language	English
Pages (from-to)	582-595
Number of pages	14
Journal	American Journal of Human Genetics
Volume	77
Issue number	4
DOIs	https://doi.org/10.1086/491603
State	Published - Oct 2005

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McQueen, M. B., Devlin, B., Faraone, S. V., Nimgaonkar, V. L., Sklar, P., Smoller, J. W., Jamra, R. A., Albus, M., Bacanu, S. A., Baron, M., Barrett, T. B., Berrettini, W., Blacker, D., Byerley, W., Cichon, S., Coryell, W., Craddock, N., Daly, M. J., DePaulo, J. R., ... Laird, N. M. (2005). Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q. American Journal of Human Genetics, 77(4), 582-595. https://doi.org/10.1086/491603

@article{df280281afcd4334ad15cf2047c17ed8,

title = "Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q",

abstract = "Several independent studies and meta-analyses aimed at identifying genomic regions linked to bipolar disorder (BP) have failed to find clear and consistent evidence of linkage regions. Our hypothesis is that combining the original genotype data provides benefits of increased power and control over sources of heterogeneity that outweigh the difficulty and potential pitfalls of the implementation. We conducted a combined analysis using the original genotype data from 11 BP genomewide linkage scans comprising 5,179 individuals from 1,067 families. Heterogeneity among studies was minimized in our analyses by using uniform methods of analysis and a common, standardized marker map and was assessed using novel methods developed for meta-analysis of genome scans. To date, this collaboration is the largest and most comprehensive analysis of linkage samples involving a psychiatric disorder. We demonstrate that combining original genome-scan data is a powerful approach for the elucidation of linkage regions underlying complex disease. Our results establish genomewide significant linkage to BP on chromosomes 6q and 8q, which provides solid information to guide future gene-finding efforts that rely on fine-mapping and association approaches.",

author = "McQueen, \{Matthew B.\} and B. Devlin and Faraone, \{Stephen V.\} and Nimgaonkar, \{Vishwajit L.\} and Pamela Sklar and Smoller, \{Jordan W.\} and Jamra, \{Rami Abou\} and Margot Albus and Bacanu, \{Silviu Alin\} and Miron Baron and Barrett, \{Thomas B.\} and Wade Berrettini and Deborah Blacker and William Byerley and Sven Cichon and Willam Coryell and Nick Craddock and Daly, \{Mark J.\} and DePaulo, \{J. Raymond\} and Edenberg, \{Howard J.\} and Tatiana Foroud and Michael Gill and Gilliam, \{T. Conrad\} and Marian Hamshere and Ian Jones and Lisa Jones and Juo, \{Suh Hang\} and Kelsoe, \{John R.\} and David Lambert and Christoph Lange and Bernard Lerer and Jianjun Liu and Wolfgang Maier and MacKinnon, \{James D.\} and McInnis, \{Melvin G.\} and McMahon, \{Francis J.\} and Murphy, \{Dennis L.\} and N{\"o}then, \{Markus M.\} and Nurnberger, \{John I.\} and Pato, \{Carlos N.\} and Pato, \{Michele T.\} and Potash, \{James B.\} and Peter Propping and Pulver, \{Ann E.\} and Rice, \{John P.\} and Marcella Rietschel and William Scheftner and Johannes Schumacher and Ricardo Segurado and \{Van Steen\}, Kristel and Weiting Xie and Zandi, \{Peter P.\} and Laird, \{Nan M.\}",

year = "2005",

month = oct,

doi = "10.1086/491603",

language = "English",

volume = "77",

pages = "582--595",

journal = "American Journal of Human Genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "4",

}

McQueen, MB, Devlin, B, Faraone, SV, Nimgaonkar, VL, Sklar, P, Smoller, JW, Jamra, RA, Albus, M, Bacanu, SA, Baron, M, Barrett, TB, Berrettini, W, Blacker, D, Byerley, W, Cichon, S, Coryell, W, Craddock, N, Daly, MJ, DePaulo, JR, Edenberg, HJ, Foroud, T, Gill, M, Gilliam, TC, Hamshere, M, Jones, I, Jones, L, Juo, SH, Kelsoe, JR, Lambert, D, Lange, C, Lerer, B, Liu, J, Maier, W, MacKinnon, JD, McInnis, MG, McMahon, FJ, Murphy, DL, Nöthen, MM, Nurnberger, JI, Pato, CN, Pato, MT, Potash, JB, Propping, P, Pulver, AE, Rice, JP, Rietschel, M, Scheftner, W, Schumacher, J, Segurado, R, Van Steen, K, Xie, W, Zandi, PP & Laird, NM 2005, 'Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q', American Journal of Human Genetics, vol. 77, no. 4, pp. 582-595. https://doi.org/10.1086/491603

TY - JOUR

T1 - Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q

AU - McQueen, Matthew B.

AU - Devlin, B.

AU - Faraone, Stephen V.

AU - Nimgaonkar, Vishwajit L.

AU - Sklar, Pamela

AU - Smoller, Jordan W.

AU - Jamra, Rami Abou

AU - Albus, Margot

AU - Bacanu, Silviu Alin

AU - Baron, Miron

AU - Barrett, Thomas B.

AU - Berrettini, Wade

AU - Blacker, Deborah

AU - Byerley, William

AU - Cichon, Sven

AU - Coryell, Willam

AU - Craddock, Nick

AU - Daly, Mark J.

AU - DePaulo, J. Raymond

AU - Edenberg, Howard J.

AU - Foroud, Tatiana

AU - Gill, Michael

AU - Gilliam, T. Conrad

AU - Hamshere, Marian

AU - Jones, Ian

AU - Jones, Lisa

AU - Juo, Suh Hang

AU - Kelsoe, John R.

AU - Lambert, David

AU - Lange, Christoph

AU - Lerer, Bernard

AU - Liu, Jianjun

AU - Maier, Wolfgang

AU - MacKinnon, James D.

AU - McInnis, Melvin G.

AU - McMahon, Francis J.

AU - Murphy, Dennis L.

AU - Nöthen, Markus M.

AU - Nurnberger, John I.

AU - Pato, Carlos N.

AU - Pato, Michele T.

AU - Potash, James B.

AU - Propping, Peter

AU - Pulver, Ann E.

AU - Rice, John P.

AU - Rietschel, Marcella

AU - Scheftner, William

AU - Schumacher, Johannes

AU - Segurado, Ricardo

AU - Van Steen, Kristel

AU - Xie, Weiting

AU - Zandi, Peter P.

AU - Laird, Nan M.

PY - 2005/10

Y1 - 2005/10

N2 - Several independent studies and meta-analyses aimed at identifying genomic regions linked to bipolar disorder (BP) have failed to find clear and consistent evidence of linkage regions. Our hypothesis is that combining the original genotype data provides benefits of increased power and control over sources of heterogeneity that outweigh the difficulty and potential pitfalls of the implementation. We conducted a combined analysis using the original genotype data from 11 BP genomewide linkage scans comprising 5,179 individuals from 1,067 families. Heterogeneity among studies was minimized in our analyses by using uniform methods of analysis and a common, standardized marker map and was assessed using novel methods developed for meta-analysis of genome scans. To date, this collaboration is the largest and most comprehensive analysis of linkage samples involving a psychiatric disorder. We demonstrate that combining original genome-scan data is a powerful approach for the elucidation of linkage regions underlying complex disease. Our results establish genomewide significant linkage to BP on chromosomes 6q and 8q, which provides solid information to guide future gene-finding efforts that rely on fine-mapping and association approaches.

AB - Several independent studies and meta-analyses aimed at identifying genomic regions linked to bipolar disorder (BP) have failed to find clear and consistent evidence of linkage regions. Our hypothesis is that combining the original genotype data provides benefits of increased power and control over sources of heterogeneity that outweigh the difficulty and potential pitfalls of the implementation. We conducted a combined analysis using the original genotype data from 11 BP genomewide linkage scans comprising 5,179 individuals from 1,067 families. Heterogeneity among studies was minimized in our analyses by using uniform methods of analysis and a common, standardized marker map and was assessed using novel methods developed for meta-analysis of genome scans. To date, this collaboration is the largest and most comprehensive analysis of linkage samples involving a psychiatric disorder. We demonstrate that combining original genome-scan data is a powerful approach for the elucidation of linkage regions underlying complex disease. Our results establish genomewide significant linkage to BP on chromosomes 6q and 8q, which provides solid information to guide future gene-finding efforts that rely on fine-mapping and association approaches.

UR - https://www.scopus.com/pages/publications/25444466232

U2 - 10.1086/491603

DO - 10.1086/491603

M3 - Article

C2 - 16175504

SN - 0002-9297

VL - 77

SP - 582

EP - 595

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 4

ER -

Combined analysis from eleven linkage studies of bipolar disorder provides strong evidence of susceptibility loci on chromosomes 6q and 8q

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