Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q: Schizophrenia linkage collaborative group III

Douglas F. Levinson; Peter Holmans; Richard E. Straub; Michael J. Owen; Dieter B. Wildenauer; Pablo V. Gejman; Ann E. Pulver; Claudine Laurent; Kenneth S. Kendler; Dermot Walsh; N. Norton; Nigel M. Williams; Sibylle G. Schwab; Bernard Lerer; Bryan J. Mowry; Alan R. Sanders; Stylianos E. Antonarakis; Jean Louis Blouin; Jean Francois DeLeuze; Jacques Mallet

doi:10.1086/303041

Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q: Schizophrenia linkage collaborative group III

Douglas F. Levinson, Peter Holmans, Richard E. Straub, Michael J. Owen, Dieter B. Wildenauer, Pablo V. Gejman, Ann E. Pulver, Claudine Laurent, Kenneth S. Kendler, Dermot Walsh, N. Norton, Nigel M. Williams, Sibylle G. Schwab, Bernard Lerer, Bryan J. Mowry, Alan R. Sanders, Stylianos E. Antonarakis, Jean Louis Blouin, Jean Francois DeLeuze, Jacques Mallet

Cancer Biology

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

178 Scopus citations

Abstract

Schizophrenia candidate regions 33-51 cM in length on chromosomes 5q, 6q, 10p, and 13q were investigated for genetic linkage with mapped markers with an average spacing of 5.64 cM. We studied 734 informative multiplex pedigrees (824 independent affected sibling pairs [ASPs], or 1, 003 ASPs when all possible pairs are counted), which were collected in eight centers. Cases with diagnoses of schizophrenia or schizoaffective disorder (DSM-IIIR criteria) were considered affected (n = 1, 937). Data were analyzed with multipoint methods, including nonparametric linkage (NPL), ASP analysis using the possible-triangle method, and logistic-regression analysis of identity-by-descent (IBD) sharing in ASPs with sample as a covariate, in a test for intersample heterogeneity and for linkage with allowance for intersample heterogeneity. The data most supportive for linkage to schizophrenia were from chromosome 6q; logistic-regression analysis of linkage allowing for intersample heterogeneity produced an empirical P value < .0002 with, or P = .0004 without, inclusion of the sample that produced the first positive report in this region; the maximum NPL score in this region was 2.47 (P = .0046), the maximum LOD score (MLS) from ASP analysis was 3.10 (empirical P = .0036), and there was significant evidence for intersample heterogeneity (empirical P = .0038). More-modest support for linkage was observed for chromosome 10p, with logistic-regression analysis of linkage producing an empirical P = .045 and with significant evidence for intersample heterogeneity (empirical P = .0096).

Original language	English (US)
Pages (from-to)	652-663
Number of pages	12
Journal	American journal of human genetics
Volume	67
Issue number	3
DOIs	https://doi.org/10.1086/303041
State	Published - 2000

ASJC Scopus subject areas

Genetics
Genetics(clinical)

Access to Document

10.1086/303041

Cite this

Levinson, D. F., Holmans, P., Straub, R. E., Owen, M. J., Wildenauer, D. B., Gejman, P. V., Pulver, A. E., Laurent, C., Kendler, K. S., Walsh, D., Norton, N., Williams, N. M., Schwab, S. G., Lerer, B., Mowry, B. J., Sanders, A. R., Antonarakis, S. E., Blouin, J. L., DeLeuze, J. F., & Mallet, J. (2000). Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q: Schizophrenia linkage collaborative group III. American journal of human genetics, 67(3), 652-663. https://doi.org/10.1086/303041

Levinson, DF, Holmans, P, Straub, RE, Owen, MJ, Wildenauer, DB, Gejman, PV, Pulver, AE, Laurent, C, Kendler, KS, Walsh, D, Norton, N, Williams, NM, Schwab, SG, Lerer, B, Mowry, BJ, Sanders, AR, Antonarakis, SE, Blouin, JL, DeLeuze, JF & Mallet, J 2000, 'Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q: Schizophrenia linkage collaborative group III', American journal of human genetics, vol. 67, no. 3, pp. 652-663. https://doi.org/10.1086/303041

@article{2462ef5dbd4746d5b2ded47ac4c313f8,

title = "Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q: Schizophrenia linkage collaborative group III",

abstract = "Schizophrenia candidate regions 33-51 cM in length on chromosomes 5q, 6q, 10p, and 13q were investigated for genetic linkage with mapped markers with an average spacing of 5.64 cM. We studied 734 informative multiplex pedigrees (824 independent affected sibling pairs [ASPs], or 1, 003 ASPs when all possible pairs are counted), which were collected in eight centers. Cases with diagnoses of schizophrenia or schizoaffective disorder (DSM-IIIR criteria) were considered affected (n = 1, 937). Data were analyzed with multipoint methods, including nonparametric linkage (NPL), ASP analysis using the possible-triangle method, and logistic-regression analysis of identity-by-descent (IBD) sharing in ASPs with sample as a covariate, in a test for intersample heterogeneity and for linkage with allowance for intersample heterogeneity. The data most supportive for linkage to schizophrenia were from chromosome 6q; logistic-regression analysis of linkage allowing for intersample heterogeneity produced an empirical P value < .0002 with, or P = .0004 without, inclusion of the sample that produced the first positive report in this region; the maximum NPL score in this region was 2.47 (P = .0046), the maximum LOD score (MLS) from ASP analysis was 3.10 (empirical P = .0036), and there was significant evidence for intersample heterogeneity (empirical P = .0038). More-modest support for linkage was observed for chromosome 10p, with logistic-regression analysis of linkage producing an empirical P = .045 and with significant evidence for intersample heterogeneity (empirical P = .0096).",

author = "Levinson, {Douglas F.} and Peter Holmans and Straub, {Richard E.} and Owen, {Michael J.} and Wildenauer, {Dieter B.} and Gejman, {Pablo V.} and Pulver, {Ann E.} and Claudine Laurent and Kendler, {Kenneth S.} and Dermot Walsh and N. Norton and Williams, {Nigel M.} and Schwab, {Sibylle G.} and Bernard Lerer and Mowry, {Bryan J.} and Sanders, {Alan R.} and Antonarakis, {Stylianos E.} and Blouin, {Jean Louis} and DeLeuze, {Jean Francois} and Jacques Mallet",

note = "Funding Information: The assistance of the following collaborators is gratefully acknowledged: MCV/Ireland: F. Anthony O'Neill (The Queen's University, Belfast). U Wales: Michael O'Donovan, Alastair Cardno, Kieran Murphy, Lisa Jones, and Robert Sanders (University of Wales College of Medicine, Cardiff); Peter McGuffin (Institute of Psychiatry, London). U Bonn: Wolfgang Maier (University of Bonn); Margot Albus, (State Mental Hospital, Haar, Germany). US/Aust: Simon J. Foote and Kelly R. Ewen (Australian Genome Research Facility, Melbourne); Deborah Nertney, David Lennon, and Helen Jones (Wolston Park Hospital, Brisbane); Derek Nancarrow and Nicholas Hayward (Queensland Institute of Medical Research, Brisbane); Matthew O'Brien and Catherine Thornley (Mental Health Research Institute, Melbourne); Madeline Gladis (University of Pennsylvania); Jeremy Silverman, Richard Mohs, Larry Siever, Christopher Smith (Mt. Sinai Medical School, New York); Raymond Crowe, Donald Black and Nancy Andreasen (University of Iowa); Jean Endicott and Larry Sharpe (Columbia University, New York). U Chicago: Qiuhe Cao, Jing Zhang, Juliet J. Guroff, Mary E. Maxwell, Diane Kazuba, and Elliot S. Gershon (University of Chicago). JHU: Gerald Nestadt and staff of the JHU Epidemiology-Genetics Program in Psychiatry; Corinne Gehrig, Uppala Radhakrishna, and Genevieve Duriaux Sa{\"i}l (University of Geneva). CNRS: Stephane Soubigou, Dominique Campion, Maurice Jay, Florence Thibaut, Michel de Chaldee, and Fabienne Treilhou (CNRS). Specimens from the National Institute of Mental Health Schizophrenia Genetics Initiative (NIMH SGI) were utilized in this study, with genotyping by the US/Australia group (Australian Genome Research Facility, Drs. Foote and Ewen). Data and biomaterials were collected in three projects that participated in the NIMH-SGI. From 1991–1997, the Principal Investigators and Co-Investigators were: Harvard University, Boston, MA, U01 MH46318, Ming T. Tsuang, M.D., Ph.D., D.Sc., Stephen Faraone, Ph.D., and John Pepple, Ph.D.; Washington University, St. Louis, MO, U01 MH46276, C. Robert Cloninger, M.D., Theodore Reich, M.D., and Dragan Svrakic, M.D.; Columbia University, New York, NY U01 MH46289, Charles Kaufmann, M.D., Dolores Malaspina, M.D., and Jill Harkavy Friedman, Ph.D. Financial support for this project was provided by NIMH grants MH 41953, 52537, and 45390 (MCV/Ireland); Medical Research Council (United Kingdom) (U Wales); Deutsche Forschungsgemeinschaft (Bonn); NIMH grants MH45097 and KO201207 and the Beukenkamp Foundation (Philadelphia); National Health and Medical Research Council of Australia (NHMRC) grants 33505, 35016, Rebecca L. Cooper Medical Research Foundation, Queensland Department of Health, and NHMRC Network for Brain Research into Mental Disorders (B.J.M.); the National Institute of Mental Health Intramural Program (U Chicago); Novartis, and University Hospitals of Geneva (JHU); l'Association Francaise contre les Myopathies, and Aventis SA (CNRS). We are grateful to all of the family members and clinicians whose contributions have made this study possible. ",

year = "2000",

doi = "10.1086/303041",

language = "English (US)",

volume = "67",

pages = "652--663",

journal = "American journal of human genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "3",

}

TY - JOUR

T1 - Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q

T2 - Schizophrenia linkage collaborative group III

AU - Levinson, Douglas F.

AU - Holmans, Peter

AU - Straub, Richard E.

AU - Owen, Michael J.

AU - Wildenauer, Dieter B.

AU - Gejman, Pablo V.

AU - Pulver, Ann E.

AU - Laurent, Claudine

AU - Kendler, Kenneth S.

AU - Walsh, Dermot

AU - Norton, N.

AU - Williams, Nigel M.

AU - Schwab, Sibylle G.

AU - Lerer, Bernard

AU - Mowry, Bryan J.

AU - Sanders, Alan R.

AU - Antonarakis, Stylianos E.

AU - Blouin, Jean Louis

AU - DeLeuze, Jean Francois

AU - Mallet, Jacques

N1 - Funding Information: The assistance of the following collaborators is gratefully acknowledged: MCV/Ireland: F. Anthony O'Neill (The Queen's University, Belfast). U Wales: Michael O'Donovan, Alastair Cardno, Kieran Murphy, Lisa Jones, and Robert Sanders (University of Wales College of Medicine, Cardiff); Peter McGuffin (Institute of Psychiatry, London). U Bonn: Wolfgang Maier (University of Bonn); Margot Albus, (State Mental Hospital, Haar, Germany). US/Aust: Simon J. Foote and Kelly R. Ewen (Australian Genome Research Facility, Melbourne); Deborah Nertney, David Lennon, and Helen Jones (Wolston Park Hospital, Brisbane); Derek Nancarrow and Nicholas Hayward (Queensland Institute of Medical Research, Brisbane); Matthew O'Brien and Catherine Thornley (Mental Health Research Institute, Melbourne); Madeline Gladis (University of Pennsylvania); Jeremy Silverman, Richard Mohs, Larry Siever, Christopher Smith (Mt. Sinai Medical School, New York); Raymond Crowe, Donald Black and Nancy Andreasen (University of Iowa); Jean Endicott and Larry Sharpe (Columbia University, New York). U Chicago: Qiuhe Cao, Jing Zhang, Juliet J. Guroff, Mary E. Maxwell, Diane Kazuba, and Elliot S. Gershon (University of Chicago). JHU: Gerald Nestadt and staff of the JHU Epidemiology-Genetics Program in Psychiatry; Corinne Gehrig, Uppala Radhakrishna, and Genevieve Duriaux Saïl (University of Geneva). CNRS: Stephane Soubigou, Dominique Campion, Maurice Jay, Florence Thibaut, Michel de Chaldee, and Fabienne Treilhou (CNRS). Specimens from the National Institute of Mental Health Schizophrenia Genetics Initiative (NIMH SGI) were utilized in this study, with genotyping by the US/Australia group (Australian Genome Research Facility, Drs. Foote and Ewen). Data and biomaterials were collected in three projects that participated in the NIMH-SGI. From 1991–1997, the Principal Investigators and Co-Investigators were: Harvard University, Boston, MA, U01 MH46318, Ming T. Tsuang, M.D., Ph.D., D.Sc., Stephen Faraone, Ph.D., and John Pepple, Ph.D.; Washington University, St. Louis, MO, U01 MH46276, C. Robert Cloninger, M.D., Theodore Reich, M.D., and Dragan Svrakic, M.D.; Columbia University, New York, NY U01 MH46289, Charles Kaufmann, M.D., Dolores Malaspina, M.D., and Jill Harkavy Friedman, Ph.D. Financial support for this project was provided by NIMH grants MH 41953, 52537, and 45390 (MCV/Ireland); Medical Research Council (United Kingdom) (U Wales); Deutsche Forschungsgemeinschaft (Bonn); NIMH grants MH45097 and KO201207 and the Beukenkamp Foundation (Philadelphia); National Health and Medical Research Council of Australia (NHMRC) grants 33505, 35016, Rebecca L. Cooper Medical Research Foundation, Queensland Department of Health, and NHMRC Network for Brain Research into Mental Disorders (B.J.M.); the National Institute of Mental Health Intramural Program (U Chicago); Novartis, and University Hospitals of Geneva (JHU); l'Association Francaise contre les Myopathies, and Aventis SA (CNRS). We are grateful to all of the family members and clinicians whose contributions have made this study possible.

PY - 2000

Y1 - 2000

N2 - Schizophrenia candidate regions 33-51 cM in length on chromosomes 5q, 6q, 10p, and 13q were investigated for genetic linkage with mapped markers with an average spacing of 5.64 cM. We studied 734 informative multiplex pedigrees (824 independent affected sibling pairs [ASPs], or 1, 003 ASPs when all possible pairs are counted), which were collected in eight centers. Cases with diagnoses of schizophrenia or schizoaffective disorder (DSM-IIIR criteria) were considered affected (n = 1, 937). Data were analyzed with multipoint methods, including nonparametric linkage (NPL), ASP analysis using the possible-triangle method, and logistic-regression analysis of identity-by-descent (IBD) sharing in ASPs with sample as a covariate, in a test for intersample heterogeneity and for linkage with allowance for intersample heterogeneity. The data most supportive for linkage to schizophrenia were from chromosome 6q; logistic-regression analysis of linkage allowing for intersample heterogeneity produced an empirical P value < .0002 with, or P = .0004 without, inclusion of the sample that produced the first positive report in this region; the maximum NPL score in this region was 2.47 (P = .0046), the maximum LOD score (MLS) from ASP analysis was 3.10 (empirical P = .0036), and there was significant evidence for intersample heterogeneity (empirical P = .0038). More-modest support for linkage was observed for chromosome 10p, with logistic-regression analysis of linkage producing an empirical P = .045 and with significant evidence for intersample heterogeneity (empirical P = .0096).

AB - Schizophrenia candidate regions 33-51 cM in length on chromosomes 5q, 6q, 10p, and 13q were investigated for genetic linkage with mapped markers with an average spacing of 5.64 cM. We studied 734 informative multiplex pedigrees (824 independent affected sibling pairs [ASPs], or 1, 003 ASPs when all possible pairs are counted), which were collected in eight centers. Cases with diagnoses of schizophrenia or schizoaffective disorder (DSM-IIIR criteria) were considered affected (n = 1, 937). Data were analyzed with multipoint methods, including nonparametric linkage (NPL), ASP analysis using the possible-triangle method, and logistic-regression analysis of identity-by-descent (IBD) sharing in ASPs with sample as a covariate, in a test for intersample heterogeneity and for linkage with allowance for intersample heterogeneity. The data most supportive for linkage to schizophrenia were from chromosome 6q; logistic-regression analysis of linkage allowing for intersample heterogeneity produced an empirical P value < .0002 with, or P = .0004 without, inclusion of the sample that produced the first positive report in this region; the maximum NPL score in this region was 2.47 (P = .0046), the maximum LOD score (MLS) from ASP analysis was 3.10 (empirical P = .0036), and there was significant evidence for intersample heterogeneity (empirical P = .0038). More-modest support for linkage was observed for chromosome 10p, with logistic-regression analysis of linkage producing an empirical P = .045 and with significant evidence for intersample heterogeneity (empirical P = .0096).

UR - http://www.scopus.com/inward/record.url?scp=0033842462&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=0033842462&partnerID=8YFLogxK

U2 - 10.1086/303041

DO - 10.1086/303041

M3 - Article

C2 - 10924404

AN - SCOPUS:0033842462

SN - 0002-9297

VL - 67

SP - 652

EP - 663

JO - American journal of human genetics

JF - American journal of human genetics

IS - 3

ER -

Multicenter linkage study of schizophrenia candidate regions on chromosomes 5q, 6q, 10p, and 13q: Schizophrenia linkage collaborative group III

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this