Case-control genome-wide association study of attention-deficit/ hyperactivity disorder

Benjamin M. Neale; Sarah Medland; Stephan Ripke; Richard J.L. Anney; Philip Asherson; Jan Buitelaar; Barbara Franke; Michael Gill; Lindsey Kent; Peter Holmans; Frank Middleton; Anita Thapar; Klaus Peter Lesch; Stephen V. Faraone; Mark Daly; Thuy Trang Nguyen; Helmut Schäfer; Hans Christoph Steinhausen; Andreas Reif; Tobias J. Renner; Marcel Romanos; Jasmin Romanos; Andreas Warnke; Susanne Walitza; Christine Freitag; Jobst Meyer; Haukur Palmason; Aribert Rothenberger; Ziarih Hawi; Joseph Sergeant; Herbert Roeyers; Eric Mick; Joseph Biederman

doi:10.1016/j.jaac.2010.06.007

Case-control genome-wide association study of attention-deficit/ hyperactivity disorder

Benjamin M. Neale, Sarah Medland, Stephan Ripke, Richard J.L. Anney, Philip Asherson, Jan Buitelaar, Barbara Franke, Michael Gill, Lindsey Kent, Peter Holmans, Frank Middleton, Anita Thapar, Klaus Peter Lesch, Stephen V. Faraone, Mark Daly, Thuy Trang Nguyen, Helmut Schäfer, Hans Christoph Steinhausen, Andreas Reif, Tobias J. RennerMarcel Romanos, Jasmin Romanos, Andreas Warnke, Susanne Walitza, Christine Freitag, Jobst Meyer, Haukur Palmason, Aribert Rothenberger, Ziarih Hawi, Joseph Sergeant, Herbert Roeyers, Eric Mick, Joseph Biederman

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

145 Scopus citations

Abstract

Objective: Although twin and family studies have shown attention-deficit/ hyperactivity disorder (ADHD) to be highly heritable, genetic variants influencing the trait at a genome-wide significant level have yet to be identified. Thus additional genomewide association studies (GWAS) are needed. Method: We used case-control analyses of 896 cases with DSM-IV ADHD genotyped using the Affymetrix 5.0 array and 2,455 repository controls screened for psychotic and bipolar symptoms genotyped using Affymetrix 6.0 arrays. A consensus SNP set was imputed using BEAGLE 3.0, resulting in an analysis dataset of 1,033,244 SNPs. Data were analyzed using a generalized linear model. Results: No genome-wide significant associations were found. The most significant results implicated the following genes: PRKG1, FLNC, TCERG1L, PPM1H, NXPH1, PPM1H, CDH13, HK1, and HKDC1. Conclusions: The current analyses are a useful addition to the present literature and will make a valuable contribution to future meta-analyses. The candidate gene findings are consistent with a prior meta-analysis in suggesting that the effects of ADHD risk variants must, individually, be very small and/or include multiple rare alleles.

Original language	English
Pages (from-to)	906-920
Number of pages	15
Journal	Journal of the American Academy of Child and Adolescent Psychiatry
Volume	49
Issue number	9
DOIs	https://doi.org/10.1016/j.jaac.2010.06.007
State	Published - Sep 2010
Externally published	Yes

Keywords

ADHD
genetics
genome-wide association
imputation

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10.1016/j.jaac.2010.06.007

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Neale, B. M., Medland, S., Ripke, S., Anney, R. J. L., Asherson, P., Buitelaar, J., Franke, B., Gill, M., Kent, L., Holmans, P., Middleton, F., Thapar, A., Lesch, K. P., Faraone, S. V., Daly, M., Nguyen, T. T., Schäfer, H., Steinhausen, H. C., Reif, A., ... Biederman, J. (2010). Case-control genome-wide association study of attention-deficit/ hyperactivity disorder. Journal of the American Academy of Child and Adolescent Psychiatry, 49(9), 906-920. https://doi.org/10.1016/j.jaac.2010.06.007

@article{dd5f340062b043f5aa50e0239ff6e1a3,

title = "Case-control genome-wide association study of attention-deficit/ hyperactivity disorder",

abstract = "Objective: Although twin and family studies have shown attention-deficit/ hyperactivity disorder (ADHD) to be highly heritable, genetic variants influencing the trait at a genome-wide significant level have yet to be identified. Thus additional genomewide association studies (GWAS) are needed. Method: We used case-control analyses of 896 cases with DSM-IV ADHD genotyped using the Affymetrix 5.0 array and 2,455 repository controls screened for psychotic and bipolar symptoms genotyped using Affymetrix 6.0 arrays. A consensus SNP set was imputed using BEAGLE 3.0, resulting in an analysis dataset of 1,033,244 SNPs. Data were analyzed using a generalized linear model. Results: No genome-wide significant associations were found. The most significant results implicated the following genes: PRKG1, FLNC, TCERG1L, PPM1H, NXPH1, PPM1H, CDH13, HK1, and HKDC1. Conclusions: The current analyses are a useful addition to the present literature and will make a valuable contribution to future meta-analyses. The candidate gene findings are consistent with a prior meta-analysis in suggesting that the effects of ADHD risk variants must, individually, be very small and/or include multiple rare alleles.",

keywords = "ADHD, genetics, genome-wide association, imputation",

author = "Neale, {Benjamin M.} and Sarah Medland and Stephan Ripke and Anney, {Richard J.L.} and Philip Asherson and Jan Buitelaar and Barbara Franke and Michael Gill and Lindsey Kent and Peter Holmans and Frank Middleton and Anita Thapar and Lesch, {Klaus Peter} and Faraone, {Stephen V.} and Mark Daly and Nguyen, {Thuy Trang} and Helmut Sch{\"a}fer and Steinhausen, {Hans Christoph} and Andreas Reif and Renner, {Tobias J.} and Marcel Romanos and Jasmin Romanos and Andreas Warnke and Susanne Walitza and Christine Freitag and Jobst Meyer and Haukur Palmason and Aribert Rothenberger and Ziarih Hawi and Joseph Sergeant and Herbert Roeyers and Eric Mick and Joseph Biederman",

note = "Funding Information: This work was supported by the following grants: US National Institutes of Health grants R13MH059126 , R01MH62873 , U01MH085518 , and R01MH081803 to S.V. Faraone; Affymetrix Power Award, 2007, to B. Franke; NHMRC (Australia); a Sidney Sax Public Health Fellowship ( 443036 ) to S.E. Medland; Wellcome Trust , UK to L. Kent; an Internal Grant of Radboud University Nijmegen Medical Centre to J. Buitelaar; a Wellcome Trust , UK, grant to A. Thapar, M. O'Donovan, and M. Owen; Deutsche Forschungsgemeinschaft grant KFO 125 to K.P. Lesch and A. Reif; SFB 581 and GRK 1156 to K.P. Lesch; RE 1632/5-1 to A. Reif; SFB TRR58 to K.P. Lesch and A. Reif; ME 1923/5-1 and ME 1923/5-3 to C. Freitag and J. Meyer; SCHA 542/10-3 to H. Sch{\"a}fer; and the Bundesministerium f{\"u}r Bildung und Forschung BMBF grant 01GV0605 to K.P. Lesch. ",

year = "2010",

month = sep,

doi = "10.1016/j.jaac.2010.06.007",

language = "English",

volume = "49",

pages = "906--920",

journal = "Journal of the American Academy of Child and Adolescent Psychiatry",

issn = "0890-8567",

publisher = "Elsevier Inc.",

number = "9",

}

Neale, BM, Medland, S, Ripke, S, Anney, RJL, Asherson, P, Buitelaar, J, Franke, B, Gill, M, Kent, L, Holmans, P, Middleton, F, Thapar, A, Lesch, KP, Faraone, SV, Daly, M, Nguyen, TT, Schäfer, H, Steinhausen, HC, Reif, A, Renner, TJ, Romanos, M, Romanos, J, Warnke, A, Walitza, S, Freitag, C, Meyer, J, Palmason, H, Rothenberger, A, Hawi, Z, Sergeant, J, Roeyers, H, Mick, E & Biederman, J 2010, 'Case-control genome-wide association study of attention-deficit/ hyperactivity disorder', Journal of the American Academy of Child and Adolescent Psychiatry, vol. 49, no. 9, pp. 906-920. https://doi.org/10.1016/j.jaac.2010.06.007

TY - JOUR

T1 - Case-control genome-wide association study of attention-deficit/ hyperactivity disorder

AU - Neale, Benjamin M.

AU - Medland, Sarah

AU - Ripke, Stephan

AU - Anney, Richard J.L.

AU - Asherson, Philip

AU - Buitelaar, Jan

AU - Franke, Barbara

AU - Gill, Michael

AU - Kent, Lindsey

AU - Holmans, Peter

AU - Middleton, Frank

AU - Thapar, Anita

AU - Lesch, Klaus Peter

AU - Faraone, Stephen V.

AU - Daly, Mark

AU - Nguyen, Thuy Trang

AU - Schäfer, Helmut

AU - Steinhausen, Hans Christoph

AU - Reif, Andreas

AU - Renner, Tobias J.

AU - Romanos, Marcel

AU - Romanos, Jasmin

AU - Warnke, Andreas

AU - Walitza, Susanne

AU - Freitag, Christine

AU - Meyer, Jobst

AU - Palmason, Haukur

AU - Rothenberger, Aribert

AU - Hawi, Ziarih

AU - Sergeant, Joseph

AU - Roeyers, Herbert

AU - Mick, Eric

AU - Biederman, Joseph

N1 - Funding Information: This work was supported by the following grants: US National Institutes of Health grants R13MH059126 , R01MH62873 , U01MH085518 , and R01MH081803 to S.V. Faraone; Affymetrix Power Award, 2007, to B. Franke; NHMRC (Australia); a Sidney Sax Public Health Fellowship ( 443036 ) to S.E. Medland; Wellcome Trust , UK to L. Kent; an Internal Grant of Radboud University Nijmegen Medical Centre to J. Buitelaar; a Wellcome Trust , UK, grant to A. Thapar, M. O'Donovan, and M. Owen; Deutsche Forschungsgemeinschaft grant KFO 125 to K.P. Lesch and A. Reif; SFB 581 and GRK 1156 to K.P. Lesch; RE 1632/5-1 to A. Reif; SFB TRR58 to K.P. Lesch and A. Reif; ME 1923/5-1 and ME 1923/5-3 to C. Freitag and J. Meyer; SCHA 542/10-3 to H. Schäfer; and the Bundesministerium für Bildung und Forschung BMBF grant 01GV0605 to K.P. Lesch.

PY - 2010/9

Y1 - 2010/9

N2 - Objective: Although twin and family studies have shown attention-deficit/ hyperactivity disorder (ADHD) to be highly heritable, genetic variants influencing the trait at a genome-wide significant level have yet to be identified. Thus additional genomewide association studies (GWAS) are needed. Method: We used case-control analyses of 896 cases with DSM-IV ADHD genotyped using the Affymetrix 5.0 array and 2,455 repository controls screened for psychotic and bipolar symptoms genotyped using Affymetrix 6.0 arrays. A consensus SNP set was imputed using BEAGLE 3.0, resulting in an analysis dataset of 1,033,244 SNPs. Data were analyzed using a generalized linear model. Results: No genome-wide significant associations were found. The most significant results implicated the following genes: PRKG1, FLNC, TCERG1L, PPM1H, NXPH1, PPM1H, CDH13, HK1, and HKDC1. Conclusions: The current analyses are a useful addition to the present literature and will make a valuable contribution to future meta-analyses. The candidate gene findings are consistent with a prior meta-analysis in suggesting that the effects of ADHD risk variants must, individually, be very small and/or include multiple rare alleles.

AB - Objective: Although twin and family studies have shown attention-deficit/ hyperactivity disorder (ADHD) to be highly heritable, genetic variants influencing the trait at a genome-wide significant level have yet to be identified. Thus additional genomewide association studies (GWAS) are needed. Method: We used case-control analyses of 896 cases with DSM-IV ADHD genotyped using the Affymetrix 5.0 array and 2,455 repository controls screened for psychotic and bipolar symptoms genotyped using Affymetrix 6.0 arrays. A consensus SNP set was imputed using BEAGLE 3.0, resulting in an analysis dataset of 1,033,244 SNPs. Data were analyzed using a generalized linear model. Results: No genome-wide significant associations were found. The most significant results implicated the following genes: PRKG1, FLNC, TCERG1L, PPM1H, NXPH1, PPM1H, CDH13, HK1, and HKDC1. Conclusions: The current analyses are a useful addition to the present literature and will make a valuable contribution to future meta-analyses. The candidate gene findings are consistent with a prior meta-analysis in suggesting that the effects of ADHD risk variants must, individually, be very small and/or include multiple rare alleles.

KW - ADHD

KW - genetics

KW - genome-wide association

KW - imputation

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U2 - 10.1016/j.jaac.2010.06.007

DO - 10.1016/j.jaac.2010.06.007

M3 - Article

C2 - 20732627

AN - SCOPUS:77956180603

SN - 0890-8567

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SP - 906

EP - 920

JO - Journal of the American Academy of Child and Adolescent Psychiatry

JF - Journal of the American Academy of Child and Adolescent Psychiatry

IS - 9

ER -

Case-control genome-wide association study of attention-deficit/ hyperactivity disorder

Abstract

Keywords

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