Genome-wide association of mood-incongruent psychotic bipolar disorder.

F. S. Goes; M. L. Hamshere; F. Seifuddin; M. Pirooznia; Pamela Lynn Belmonte Mahon; R. Breuer; T. Schulze; M. Nöthen; S. Cichon; M. Rietschel; P. Holmans; P. P. Zandi; Genome Study (BiGS) Bipolar Genome Study (BiGS); N. Craddock; J. B. Potash

doi:10.1038/tp.2012.106

Genome-wide association of mood-incongruent psychotic bipolar disorder.

F. S. Goes, M. L. Hamshere, F. Seifuddin, M. Pirooznia, Pamela Lynn Belmonte Mahon, R. Breuer, T. Schulze, M. Nöthen, S. Cichon, M. Rietschel, P. Holmans, P. P. Zandi, Genome Study (BiGS) Bipolar Genome Study (BiGS), N. Craddock, J. B. Potash

School of Medicine

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44 Scopus citations

Abstract

Mood-incongruent psychotic features (MICP) are familial symptoms of bipolar disorder (BP) that also occur in schizophrenia (SZ), and may represent manifestations of shared etiology between the major psychoses. In this study we have analyzed three large samples of BP with imputed genome-wide association data and have performed a meta-analysis of 2196 cases with MICP and 8148 controls. We found several regions with suggestive evidence of association (P<10(-6)), although no marker met genome-wide significance criteria. The top associations were on chromosomes: 6q14.2 within the PRSS35/SNAP91 gene complex (rs1171113, P=9.67 × 10(-8)); 3p22.2 downstream of TRANK/LBA1 (rs9834970, P=9.71 × 10(-8)); and 14q24.2 in an intron of NUMB (rs2333194, P=7.03 × 10(-7)). These associations were present in all three samples, and both rs1171113 and rs2333194 were found to be overrepresented in an analysis of MICP cases compared with all other BP cases. To test the relationship of MICP with SZ, we performed polygenic analysis using the Psychiatric GWAS Consortium SZ results and found evidence of association between SZ polygenes and the presence of MICP in BP cases (meta-analysis P=0.003). In summary, our analysis of the MICP phenotype in BP has provided suggestive evidence for association of common variants in several genes expressed in the nervous system. The results of our polygenic analysis provides support for a modest degree of genetic overlap between BP with MICP and SZ, highlighting that phenotypic correlations across syndromes may be due to the influence of polygenic risk factors.

Original language	English (US)
Pages (from-to)	e180
Journal	Translational psychiatry
Volume	2
DOIs	https://doi.org/10.1038/tp.2012.106
State	Published - 2012

ASJC Scopus subject areas

Psychiatry and Mental health
Cellular and Molecular Neuroscience
Biological Psychiatry

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10.1038/tp.2012.106

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Goes, F. S., Hamshere, M. L., Seifuddin, F., Pirooznia, M., Mahon, P. L. B., Breuer, R., Schulze, T., Nöthen, M., Cichon, S., Rietschel, M., Holmans, P., Zandi, P. P., Bipolar Genome Study (BiGS), G. S., Craddock, N., & Potash, J. B. (2012). Genome-wide association of mood-incongruent psychotic bipolar disorder. Translational psychiatry, 2, e180. https://doi.org/10.1038/tp.2012.106

@article{cf934924ff7e458db6bd50ed007217bf,

title = "Genome-wide association of mood-incongruent psychotic bipolar disorder.",

abstract = "Mood-incongruent psychotic features (MICP) are familial symptoms of bipolar disorder (BP) that also occur in schizophrenia (SZ), and may represent manifestations of shared etiology between the major psychoses. In this study we have analyzed three large samples of BP with imputed genome-wide association data and have performed a meta-analysis of 2196 cases with MICP and 8148 controls. We found several regions with suggestive evidence of association (P<10(-6)), although no marker met genome-wide significance criteria. The top associations were on chromosomes: 6q14.2 within the PRSS35/SNAP91 gene complex (rs1171113, P=9.67 × 10(-8)); 3p22.2 downstream of TRANK/LBA1 (rs9834970, P=9.71 × 10(-8)); and 14q24.2 in an intron of NUMB (rs2333194, P=7.03 × 10(-7)). These associations were present in all three samples, and both rs1171113 and rs2333194 were found to be overrepresented in an analysis of MICP cases compared with all other BP cases. To test the relationship of MICP with SZ, we performed polygenic analysis using the Psychiatric GWAS Consortium SZ results and found evidence of association between SZ polygenes and the presence of MICP in BP cases (meta-analysis P=0.003). In summary, our analysis of the MICP phenotype in BP has provided suggestive evidence for association of common variants in several genes expressed in the nervous system. The results of our polygenic analysis provides support for a modest degree of genetic overlap between BP with MICP and SZ, highlighting that phenotypic correlations across syndromes may be due to the influence of polygenic risk factors.",

author = "Goes, {F. S.} and Hamshere, {M. L.} and F. Seifuddin and M. Pirooznia and Mahon, {Pamela Lynn Belmonte} and R. Breuer and T. Schulze and M. N{\"o}then and S. Cichon and M. Rietschel and P. Holmans and Zandi, {P. P.} and {Bipolar Genome Study (BiGS)}, {Genome Study (BiGS)} and N. Craddock and Potash, {J. B.}",

note = "Funding Information: Acknowledgements. Supported by NARSAD, NIMH (K99/R00MH086049) and the Wellcome Trust (award 076113). We express our appreciation to the families and individuals who participated in this project. We thank those involved in the BP Research Network (bdrn.org) and the MDF-The Bipolar Organization for the help of its staff and members. Funding for recruitment and phenotype assessment has been provided by the Wellcome Trust and the Medical Research Council. This study makes use of data generated by the Wellcome Trust Case–Control Consortium. A full list of the investigators who contributed to the generation of the data is available from http://www.wtccc.org.uk. The NIMH samples were genotyped under the direction of Bipolar Genome Study. The Principal Investigators and Co-Investigators were: John R Kelsoe, Tiffany A Greenwood, Caroline M Nievergelt, Rebecca McKinney, Paul D Shilling, Nicholas Schork, Erin N Smith, Cinnamon Bloss, John Nurnberger, Howard J Edenberg, Tatiana Foroud, Daniel L Koller, Elliot Gershon, Chunyu Liu, Judith A Badner, William A Scheftner, William B Lawson, Evaristus A Nwulia, Maria Hipolito, William Coryell, John Rice, William Byerley, Francis McMahon, Thomas G Schulze, David T Chen, Wade Berrettini, James B Potash, Peter P Zandi, Pamela B Mahon, Melvin G McInnis, Sebastian Z{\"o}llner, Peng Zhang, David W Craig, Szabolcs Szelinger, Thomas B Barrett.",

year = "2012",

doi = "10.1038/tp.2012.106",

language = "English (US)",

volume = "2",

pages = "e180",

journal = "Translational psychiatry",

issn = "2158-3188",

publisher = "Nature Publishing Group",

}

TY - JOUR

T1 - Genome-wide association of mood-incongruent psychotic bipolar disorder.

AU - Goes, F. S.

AU - Hamshere, M. L.

AU - Seifuddin, F.

AU - Pirooznia, M.

AU - Mahon, Pamela Lynn Belmonte

AU - Breuer, R.

AU - Schulze, T.

AU - Nöthen, M.

AU - Cichon, S.

AU - Rietschel, M.

AU - Holmans, P.

AU - Zandi, P. P.

AU - Bipolar Genome Study (BiGS), Genome Study (BiGS)

AU - Craddock, N.

AU - Potash, J. B.

N1 - Funding Information: Acknowledgements. Supported by NARSAD, NIMH (K99/R00MH086049) and the Wellcome Trust (award 076113). We express our appreciation to the families and individuals who participated in this project. We thank those involved in the BP Research Network (bdrn.org) and the MDF-The Bipolar Organization for the help of its staff and members. Funding for recruitment and phenotype assessment has been provided by the Wellcome Trust and the Medical Research Council. This study makes use of data generated by the Wellcome Trust Case–Control Consortium. A full list of the investigators who contributed to the generation of the data is available from http://www.wtccc.org.uk. The NIMH samples were genotyped under the direction of Bipolar Genome Study. The Principal Investigators and Co-Investigators were: John R Kelsoe, Tiffany A Greenwood, Caroline M Nievergelt, Rebecca McKinney, Paul D Shilling, Nicholas Schork, Erin N Smith, Cinnamon Bloss, John Nurnberger, Howard J Edenberg, Tatiana Foroud, Daniel L Koller, Elliot Gershon, Chunyu Liu, Judith A Badner, William A Scheftner, William B Lawson, Evaristus A Nwulia, Maria Hipolito, William Coryell, John Rice, William Byerley, Francis McMahon, Thomas G Schulze, David T Chen, Wade Berrettini, James B Potash, Peter P Zandi, Pamela B Mahon, Melvin G McInnis, Sebastian Zöllner, Peng Zhang, David W Craig, Szabolcs Szelinger, Thomas B Barrett.

PY - 2012

Y1 - 2012

N2 - Mood-incongruent psychotic features (MICP) are familial symptoms of bipolar disorder (BP) that also occur in schizophrenia (SZ), and may represent manifestations of shared etiology between the major psychoses. In this study we have analyzed three large samples of BP with imputed genome-wide association data and have performed a meta-analysis of 2196 cases with MICP and 8148 controls. We found several regions with suggestive evidence of association (P<10(-6)), although no marker met genome-wide significance criteria. The top associations were on chromosomes: 6q14.2 within the PRSS35/SNAP91 gene complex (rs1171113, P=9.67 × 10(-8)); 3p22.2 downstream of TRANK/LBA1 (rs9834970, P=9.71 × 10(-8)); and 14q24.2 in an intron of NUMB (rs2333194, P=7.03 × 10(-7)). These associations were present in all three samples, and both rs1171113 and rs2333194 were found to be overrepresented in an analysis of MICP cases compared with all other BP cases. To test the relationship of MICP with SZ, we performed polygenic analysis using the Psychiatric GWAS Consortium SZ results and found evidence of association between SZ polygenes and the presence of MICP in BP cases (meta-analysis P=0.003). In summary, our analysis of the MICP phenotype in BP has provided suggestive evidence for association of common variants in several genes expressed in the nervous system. The results of our polygenic analysis provides support for a modest degree of genetic overlap between BP with MICP and SZ, highlighting that phenotypic correlations across syndromes may be due to the influence of polygenic risk factors.

AB - Mood-incongruent psychotic features (MICP) are familial symptoms of bipolar disorder (BP) that also occur in schizophrenia (SZ), and may represent manifestations of shared etiology between the major psychoses. In this study we have analyzed three large samples of BP with imputed genome-wide association data and have performed a meta-analysis of 2196 cases with MICP and 8148 controls. We found several regions with suggestive evidence of association (P<10(-6)), although no marker met genome-wide significance criteria. The top associations were on chromosomes: 6q14.2 within the PRSS35/SNAP91 gene complex (rs1171113, P=9.67 × 10(-8)); 3p22.2 downstream of TRANK/LBA1 (rs9834970, P=9.71 × 10(-8)); and 14q24.2 in an intron of NUMB (rs2333194, P=7.03 × 10(-7)). These associations were present in all three samples, and both rs1171113 and rs2333194 were found to be overrepresented in an analysis of MICP cases compared with all other BP cases. To test the relationship of MICP with SZ, we performed polygenic analysis using the Psychiatric GWAS Consortium SZ results and found evidence of association between SZ polygenes and the presence of MICP in BP cases (meta-analysis P=0.003). In summary, our analysis of the MICP phenotype in BP has provided suggestive evidence for association of common variants in several genes expressed in the nervous system. The results of our polygenic analysis provides support for a modest degree of genetic overlap between BP with MICP and SZ, highlighting that phenotypic correlations across syndromes may be due to the influence of polygenic risk factors.

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JO - Translational psychiatry

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ER -

Genome-wide association of mood-incongruent psychotic bipolar disorder.

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