Family-based association of FKBP5 in bipolar disorder

V. L. Willour; H. Chen; J. Toolan; P. Belmonte; D. J. Cutler; F. S. Goes; Peter P. Zandi; R. S. Lee; Dean F. MacKinnon; F. M. Mondimore; B. Schweizer; J. Raymond DePaulo; Elliot Gershon; F. J. McMahon; James B. Potash; Erin Miller; Justin Pearl; Layla Kassem; Victor Lopez; John Nurnberger; Marvin J. Miller; Elizabeth S. Bowman; Theodore Reich; Allison Goate; John Rice; Colin Stine; Diane Kazuba; Elizabeth Maxwell; N. Leela Rau; P. Ryan Moe; Nalini Samavedy; Rif El-Mallakh; Husseini Manji; Debra A. Glitz; Eric T. Meyer; Carrie Smiley; Tatiana Foroud; Leah Flury; Danielle M. Dick; Howard Edenberg; Laura Bierut; Melvin McInnis; Dimitrios Avramopoulos; Jennifer Payne; Wade Berrettini; William Byerley; Mark Vawter; William Coryell; Raymond Crowe; Judith Badner; Chunyu Liu; Alan Sanders; Maria Caserta; Steven Dinwiddie; Tu Nguyen; Donna Harakal; John Kelsoe; Rebecca McKinney; William Scheftner; Howard M. Kravitz; Diana Marta; Annette Vaughn-Brown; Laurie Bederow; Sevilla Detera-Wadleigh; Lisa Austin; Dennis L. Murphy

doi:10.1038/sj.mp.4002141

Family-based association of FKBP5 in bipolar disorder

V. L. Willour, H. Chen, J. Toolan, P. Belmonte, D. J. Cutler, F. S. Goes, Peter P. Zandi, R. S. Lee, Dean F. MacKinnon, F. M. Mondimore, B. Schweizer, J. Raymond DePaulo, Elliot Gershon, F. J. McMahon, James B. Potash, Erin Miller, Justin Pearl, Layla Kassem, Victor Lopez, John NurnbergerMarvin J. Miller, Elizabeth S. Bowman, Theodore Reich, Allison Goate, John Rice, Colin Stine, Diane Kazuba, Elizabeth Maxwell, N. Leela Rau, P. Ryan Moe, Nalini Samavedy, Rif El-Mallakh, Husseini Manji, Debra A. Glitz, Eric T. Meyer, Carrie Smiley, Tatiana Foroud, Leah Flury, Danielle M. Dick, Howard Edenberg, Laura Bierut, Melvin McInnis, Dimitrios Avramopoulos, Jennifer Payne, Wade Berrettini, William Byerley, Mark Vawter, William Coryell, Raymond Crowe, Judith Badner, Chunyu Liu, Alan Sanders, Maria Caserta, Steven Dinwiddie, Tu Nguyen, Donna Harakal, John Kelsoe, Rebecca McKinney, William Scheftner, Howard M. Kravitz, Diana Marta, Annette Vaughn-Brown, Laurie Bederow, Sevilla Detera-Wadleigh, Lisa Austin, Dennis L. Murphy

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

143 Scopus citations

Abstract

The FKBP5 gene product forms part of a complex with the glucocorticoid receptor and can modulate cortisol-binding affinity. Variations in the gene have been associated with increased recurrence of depression and with rapid response to antidepressant treatment. We sought to determine whether common FKBP5 variants confer risk for bipolar disorder. We genotyped seven tag single-nucleotide polymorphisms (SNPs) in FKBP5, plus two SNPs previously associated with illness, in 317 families with 554 bipolar offspring, derived primarily from two studies. Single marker and haplotypic analyses were carried out with FBAT and EATDT employing the standard bipolar phenotype. Association analyses were also conducted using 11 disease-related variables as covariates. Under an additive genetic model, rs4713902 showed significant overtransmission of the major allele (P=0.0001), which was consistent across the two sample sets (P=0.004 and 0.006). rs7757037 showed evidence of association that was strongest under the dominant model (P=0.001). This result was consistent across the two datasets (P=0.017 and 0.019). The dominant model yielded modest evidence for association (P<0.05) for three additional markers. Covariate-based analyses suggested that genetic variation within FKBP5 may influence attempted suicide and number of depressive episodes in bipolar subjects. Our results are consistent with the well-established relationship between the hypothalamic-pituitary-adrenal (HPA) axis, which mediates the stress response through regulation of cortisol, and mood disorders. Ongoing whole-genome association studies in bipolar disorder and major depression should further clarify the role of FKBP5 and other HPA genes in these illnesses.

Original language	English
Pages (from-to)	261-268
Number of pages	8
Journal	Molecular Psychiatry
Volume	14
Issue number	3
DOIs	https://doi.org/10.1038/sj.mp.4002141
State	Published - Jan 1 2009

Keywords

HPA axis
Linkage disequilibrium
Mood disorder

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10.1038/sj.mp.4002141

Cite this

Willour, V. L., Chen, H., Toolan, J., Belmonte, P., Cutler, D. J., Goes, F. S., Zandi, P. P., Lee, R. S., MacKinnon, D. F., Mondimore, F. M., Schweizer, B., DePaulo, J. R., Gershon, E., McMahon, F. J., Potash, J. B., Miller, E., Pearl, J., Kassem, L., Lopez, V., ... Murphy, D. L. (2009). Family-based association of FKBP5 in bipolar disorder. Molecular Psychiatry, 14(3), 261-268. https://doi.org/10.1038/sj.mp.4002141

@article{95726f04dbe9432fb3286aa93a2c96a2,

title = "Family-based association of FKBP5 in bipolar disorder",

abstract = "The FKBP5 gene product forms part of a complex with the glucocorticoid receptor and can modulate cortisol-binding affinity. Variations in the gene have been associated with increased recurrence of depression and with rapid response to antidepressant treatment. We sought to determine whether common FKBP5 variants confer risk for bipolar disorder. We genotyped seven tag single-nucleotide polymorphisms (SNPs) in FKBP5, plus two SNPs previously associated with illness, in 317 families with 554 bipolar offspring, derived primarily from two studies. Single marker and haplotypic analyses were carried out with FBAT and EATDT employing the standard bipolar phenotype. Association analyses were also conducted using 11 disease-related variables as covariates. Under an additive genetic model, rs4713902 showed significant overtransmission of the major allele (P=0.0001), which was consistent across the two sample sets (P=0.004 and 0.006). rs7757037 showed evidence of association that was strongest under the dominant model (P=0.001). This result was consistent across the two datasets (P=0.017 and 0.019). The dominant model yielded modest evidence for association (P<0.05) for three additional markers. Covariate-based analyses suggested that genetic variation within FKBP5 may influence attempted suicide and number of depressive episodes in bipolar subjects. Our results are consistent with the well-established relationship between the hypothalamic-pituitary-adrenal (HPA) axis, which mediates the stress response through regulation of cortisol, and mood disorders. Ongoing whole-genome association studies in bipolar disorder and major depression should further clarify the role of FKBP5 and other HPA genes in these illnesses.",

keywords = "HPA axis, Linkage disequilibrium, Mood disorder",

author = "Willour, {V. L.} and H. Chen and J. Toolan and P. Belmonte and Cutler, {D. J.} and Goes, {F. S.} and Zandi, {Peter P.} and Lee, {R. S.} and MacKinnon, {Dean F.} and Mondimore, {F. M.} and B. Schweizer and DePaulo, {J. Raymond} and Elliot Gershon and McMahon, {F. J.} and Potash, {James B.} and Erin Miller and Justin Pearl and Layla Kassem and Victor Lopez and John Nurnberger and Miller, {Marvin J.} and Bowman, {Elizabeth S.} and Theodore Reich and Allison Goate and John Rice and Colin Stine and Diane Kazuba and Elizabeth Maxwell and Rau, {N. Leela} and Moe, {P. Ryan} and Nalini Samavedy and Rif El-Mallakh and Husseini Manji and Glitz, {Debra A.} and Meyer, {Eric T.} and Carrie Smiley and Tatiana Foroud and Leah Flury and Dick, {Danielle M.} and Howard Edenberg and Laura Bierut and Melvin McInnis and Dimitrios Avramopoulos and Jennifer Payne and Wade Berrettini and William Byerley and Mark Vawter and William Coryell and Raymond Crowe and Judith Badner and Chunyu Liu and Alan Sanders and Maria Caserta and Steven Dinwiddie and Tu Nguyen and Donna Harakal and John Kelsoe and Rebecca McKinney and William Scheftner and Kravitz, {Howard M.} and Diana Marta and Annette Vaughn-Brown and Laurie Bederow and Sevilla Detera-Wadleigh and Lisa Austin and Murphy, {Dennis L.}",

note = "Funding Information: This work was supported by grants from the National Institute of Mental Health (R01 MH-042243 and R01 MH-061613), the Charles A Dana Foundation Consortium on the Genetic Basis of Manic Depressive Illness, the National Alliance for Research on Schizophrenia and Depression, the Alex Brown Foundation and the Stanley Medical Research Institute. Dr Willour and Dr Potash were also supported by Margaret Ann Price Investigatorships. Some DNA samples were prepared and distributed by Rutgers University under a contract from the NIMH. We are grateful to Yuqing Huo, Kuangyi Miao and Brandie Craighead for their contributions. We are also grateful to the many interviewers and diagnosticians who contributed to this project, and to the families who devoted their time and effort to the study. The Bipolar Disorder Phenome Group consists of Francis McMahon, Jo Steele, Justin Pearl, Layla Kassem, Victor Lopez from the Genetic Basis of Mood and Anxiety Disorders Unit, Mood and Anxiety Program, National Institute of Mental Health, National Institutes of Health, Bethesda, MD; James Potash, Dean MacKinnon, Erin Miller, Jennifer Toolan from the Department of Psychiatry, Johns Hopkins School of Medicine, Baltimore, MD; Peter Zandi from the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD; Thomas Schulze from the Division of Genetic Epidemiology in Psychiatry, Central Institute of Mental Health, Ruprecht-Karls-University of Heidelberg, Mannheim, Germany; Evaristus Nwulia from the Department of Psychiatry, Howard University Hospital, Washington, DC; Sylvia Simpson from the Department of Psychiatry, University of Colorado at Denver, Denver, CO. Some of the data and biomaterials were collected in four projects that participated in the NIMH Bipolar Disorder Genetics Initiative from 1991–1998. The Principal Investigators and Co-Investigators were Indiana University, Indianapolis, IN, U01 MH46282, John Nurnberger, MD, PhD, Marvin Miller, MD and Elizabeth Bowman, MD; Washington University, St Louis, MO, U01 MH46280, Theodore Reich, MD, Allison Goate, PhD and John Rice, PhD; Johns Hopkins University, Baltimore, MD U01 MH46274, J Raymond DePaulo, Jr, MD, Sylvia Simpson, MD, MPH and Colin Stine, PhD; NIMH Intramural Research Program, Clinical Neurogenetics Branch, Bethesda, MD, Elliot Gershon, MD, Diane Kazuba, BA and Elizabeth Maxwell, MSW. Other data and biomaterials were collected in 10 NIMH Bipolar Disorder Genetics Initiative projects from 1999–2003. The Principal Investigators and Co-Investigators were Indiana University, Indianapolis, IN, R01 MH59545, John Nurnberger, MD, PhD, Marvin J Miller, MD, Elizabeth S Bowman, MD, N Leela Rau, MD, P Ryan Moe, MD, Nalini Samavedy, MD, Rif El-Mallakh, MD (at University of Louisville), Husseini Manji, MD (at Wayne State University), Debra A Glitz, MD (at Wayne State University), Eric T Meyer, MS, Carrie Smiley, RN, Tatiana Foroud, PhD, Leah Flury, MS, Danielle M Dick, PhD, Howard Edenberg, PhD; Washington University, St Louis, MO, R01 MH059534, John Rice, PhD, Theodore Reich, MD, Allison Goate, PhD, Laura Bierut, MD; Johns Hopkins University, Baltimore, MD, R01 MH59533, Melvin McInnis MD, J. Raymond DePaulo, Jr, MD, Dean F MacKinnon, MD, Francis M Mondimore, MD, James B Potash, MD, Peter P Zandi, PhD, Dimitrios Avramopoulos, PhD and Jennifer Payne, MD; University of Pennsylvania, PA, R01 MH59553, Wade Berrettini MD, PhD; University of California at Irvine, CA, R01 MH60068, William Byerley MD and Mark Vawter MD; University of Iowa, IA, R01 MH059548, William Coryell MD and Raymond Crowe MD; University of Chicago, IL, R01 MH59535, Elliot Gershon, MD, Judith Badner PhD, Francis McMahon MD, Chunyu Liu PhD, Alan Sanders MD, Maria Caserta, Steven Dinwiddie MD, Tu Nguyen, Donna Harakal; University of California at San Diego, CA, R01 MH59567, John Kelsoe, MD, Rebecca McKinney, BA; Rush University, IL, R01 MH059556, William Scheftner MD, Howard M Kravitz, DO, MPH, Diana Marta, BS, Annette Vaughn-Brown, MSN, RN and Laurie Bederow, MA; NIMH Intramural Research Program, Bethesda, MD, 1Z01MH002810-01, Francis J McMahon, MD, Layla Kassem, PsyD, Sevilla Detera-Wadleigh, PhD, Lisa Austin, PhD, Dennis L Murphy, MD.",

year = "2009",

month = jan,

day = "1",

doi = "10.1038/sj.mp.4002141",

language = "English",

volume = "14",

pages = "261--268",

journal = "Molecular Psychiatry",

issn = "1359-4184",

number = "3",

}

Willour, VL, Chen, H, Toolan, J, Belmonte, P, Cutler, DJ, Goes, FS, Zandi, PP, Lee, RS, MacKinnon, DF, Mondimore, FM, Schweizer, B, DePaulo, JR, Gershon, E, McMahon, FJ, Potash, JB, Miller, E, Pearl, J, Kassem, L, Lopez, V, Nurnberger, J, Miller, MJ, Bowman, ES, Reich, T, Goate, A, Rice, J, Stine, C, Kazuba, D, Maxwell, E, Rau, NL, Moe, PR, Samavedy, N, El-Mallakh, R, Manji, H, Glitz, DA, Meyer, ET, Smiley, C, Foroud, T, Flury, L, Dick, DM, Edenberg, H, Bierut, L, McInnis, M, Avramopoulos, D, Payne, J, Berrettini, W, Byerley, W, Vawter, M, Coryell, W, Crowe, R, Badner, J, Liu, C, Sanders, A, Caserta, M, Dinwiddie, S, Nguyen, T, Harakal, D, Kelsoe, J, McKinney, R, Scheftner, W, Kravitz, HM, Marta, D, Vaughn-Brown, A, Bederow, L, Detera-Wadleigh, S, Austin, L & Murphy, DL 2009, 'Family-based association of FKBP5 in bipolar disorder', Molecular Psychiatry, vol. 14, no. 3, pp. 261-268. https://doi.org/10.1038/sj.mp.4002141

TY - JOUR

T1 - Family-based association of FKBP5 in bipolar disorder

AU - Willour, V. L.

AU - Chen, H.

AU - Toolan, J.

AU - Belmonte, P.

AU - Cutler, D. J.

AU - Goes, F. S.

AU - Zandi, Peter P.

AU - Lee, R. S.

AU - MacKinnon, Dean F.

AU - Mondimore, F. M.

AU - Schweizer, B.

AU - DePaulo, J. Raymond

AU - Gershon, Elliot

AU - McMahon, F. J.

AU - Potash, James B.

AU - Miller, Erin

AU - Pearl, Justin

AU - Kassem, Layla

AU - Lopez, Victor

AU - Nurnberger, John

AU - Miller, Marvin J.

AU - Bowman, Elizabeth S.

AU - Reich, Theodore

AU - Goate, Allison

AU - Rice, John

AU - Stine, Colin

AU - Kazuba, Diane

AU - Maxwell, Elizabeth

AU - Rau, N. Leela

AU - Moe, P. Ryan

AU - Samavedy, Nalini

AU - El-Mallakh, Rif

AU - Manji, Husseini

AU - Glitz, Debra A.

AU - Meyer, Eric T.

AU - Smiley, Carrie

AU - Foroud, Tatiana

AU - Flury, Leah

AU - Dick, Danielle M.

AU - Edenberg, Howard

AU - Bierut, Laura

AU - McInnis, Melvin

AU - Avramopoulos, Dimitrios

AU - Payne, Jennifer

AU - Berrettini, Wade

AU - Byerley, William

AU - Vawter, Mark

AU - Coryell, William

AU - Crowe, Raymond

AU - Badner, Judith

AU - Liu, Chunyu

AU - Sanders, Alan

AU - Caserta, Maria

AU - Dinwiddie, Steven

AU - Nguyen, Tu

AU - Harakal, Donna

AU - Kelsoe, John

AU - McKinney, Rebecca

AU - Scheftner, William

AU - Kravitz, Howard M.

AU - Marta, Diana

AU - Vaughn-Brown, Annette

AU - Bederow, Laurie

AU - Detera-Wadleigh, Sevilla

AU - Austin, Lisa

AU - Murphy, Dennis L.

N1 - Funding Information: This work was supported by grants from the National Institute of Mental Health (R01 MH-042243 and R01 MH-061613), the Charles A Dana Foundation Consortium on the Genetic Basis of Manic Depressive Illness, the National Alliance for Research on Schizophrenia and Depression, the Alex Brown Foundation and the Stanley Medical Research Institute. Dr Willour and Dr Potash were also supported by Margaret Ann Price Investigatorships. Some DNA samples were prepared and distributed by Rutgers University under a contract from the NIMH. We are grateful to Yuqing Huo, Kuangyi Miao and Brandie Craighead for their contributions. We are also grateful to the many interviewers and diagnosticians who contributed to this project, and to the families who devoted their time and effort to the study. The Bipolar Disorder Phenome Group consists of Francis McMahon, Jo Steele, Justin Pearl, Layla Kassem, Victor Lopez from the Genetic Basis of Mood and Anxiety Disorders Unit, Mood and Anxiety Program, National Institute of Mental Health, National Institutes of Health, Bethesda, MD; James Potash, Dean MacKinnon, Erin Miller, Jennifer Toolan from the Department of Psychiatry, Johns Hopkins School of Medicine, Baltimore, MD; Peter Zandi from the Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD; Thomas Schulze from the Division of Genetic Epidemiology in Psychiatry, Central Institute of Mental Health, Ruprecht-Karls-University of Heidelberg, Mannheim, Germany; Evaristus Nwulia from the Department of Psychiatry, Howard University Hospital, Washington, DC; Sylvia Simpson from the Department of Psychiatry, University of Colorado at Denver, Denver, CO. Some of the data and biomaterials were collected in four projects that participated in the NIMH Bipolar Disorder Genetics Initiative from 1991–1998. The Principal Investigators and Co-Investigators were Indiana University, Indianapolis, IN, U01 MH46282, John Nurnberger, MD, PhD, Marvin Miller, MD and Elizabeth Bowman, MD; Washington University, St Louis, MO, U01 MH46280, Theodore Reich, MD, Allison Goate, PhD and John Rice, PhD; Johns Hopkins University, Baltimore, MD U01 MH46274, J Raymond DePaulo, Jr, MD, Sylvia Simpson, MD, MPH and Colin Stine, PhD; NIMH Intramural Research Program, Clinical Neurogenetics Branch, Bethesda, MD, Elliot Gershon, MD, Diane Kazuba, BA and Elizabeth Maxwell, MSW. Other data and biomaterials were collected in 10 NIMH Bipolar Disorder Genetics Initiative projects from 1999–2003. The Principal Investigators and Co-Investigators were Indiana University, Indianapolis, IN, R01 MH59545, John Nurnberger, MD, PhD, Marvin J Miller, MD, Elizabeth S Bowman, MD, N Leela Rau, MD, P Ryan Moe, MD, Nalini Samavedy, MD, Rif El-Mallakh, MD (at University of Louisville), Husseini Manji, MD (at Wayne State University), Debra A Glitz, MD (at Wayne State University), Eric T Meyer, MS, Carrie Smiley, RN, Tatiana Foroud, PhD, Leah Flury, MS, Danielle M Dick, PhD, Howard Edenberg, PhD; Washington University, St Louis, MO, R01 MH059534, John Rice, PhD, Theodore Reich, MD, Allison Goate, PhD, Laura Bierut, MD; Johns Hopkins University, Baltimore, MD, R01 MH59533, Melvin McInnis MD, J. Raymond DePaulo, Jr, MD, Dean F MacKinnon, MD, Francis M Mondimore, MD, James B Potash, MD, Peter P Zandi, PhD, Dimitrios Avramopoulos, PhD and Jennifer Payne, MD; University of Pennsylvania, PA, R01 MH59553, Wade Berrettini MD, PhD; University of California at Irvine, CA, R01 MH60068, William Byerley MD and Mark Vawter MD; University of Iowa, IA, R01 MH059548, William Coryell MD and Raymond Crowe MD; University of Chicago, IL, R01 MH59535, Elliot Gershon, MD, Judith Badner PhD, Francis McMahon MD, Chunyu Liu PhD, Alan Sanders MD, Maria Caserta, Steven Dinwiddie MD, Tu Nguyen, Donna Harakal; University of California at San Diego, CA, R01 MH59567, John Kelsoe, MD, Rebecca McKinney, BA; Rush University, IL, R01 MH059556, William Scheftner MD, Howard M Kravitz, DO, MPH, Diana Marta, BS, Annette Vaughn-Brown, MSN, RN and Laurie Bederow, MA; NIMH Intramural Research Program, Bethesda, MD, 1Z01MH002810-01, Francis J McMahon, MD, Layla Kassem, PsyD, Sevilla Detera-Wadleigh, PhD, Lisa Austin, PhD, Dennis L Murphy, MD.

PY - 2009/1/1

Y1 - 2009/1/1

N2 - The FKBP5 gene product forms part of a complex with the glucocorticoid receptor and can modulate cortisol-binding affinity. Variations in the gene have been associated with increased recurrence of depression and with rapid response to antidepressant treatment. We sought to determine whether common FKBP5 variants confer risk for bipolar disorder. We genotyped seven tag single-nucleotide polymorphisms (SNPs) in FKBP5, plus two SNPs previously associated with illness, in 317 families with 554 bipolar offspring, derived primarily from two studies. Single marker and haplotypic analyses were carried out with FBAT and EATDT employing the standard bipolar phenotype. Association analyses were also conducted using 11 disease-related variables as covariates. Under an additive genetic model, rs4713902 showed significant overtransmission of the major allele (P=0.0001), which was consistent across the two sample sets (P=0.004 and 0.006). rs7757037 showed evidence of association that was strongest under the dominant model (P=0.001). This result was consistent across the two datasets (P=0.017 and 0.019). The dominant model yielded modest evidence for association (P<0.05) for three additional markers. Covariate-based analyses suggested that genetic variation within FKBP5 may influence attempted suicide and number of depressive episodes in bipolar subjects. Our results are consistent with the well-established relationship between the hypothalamic-pituitary-adrenal (HPA) axis, which mediates the stress response through regulation of cortisol, and mood disorders. Ongoing whole-genome association studies in bipolar disorder and major depression should further clarify the role of FKBP5 and other HPA genes in these illnesses.

AB - The FKBP5 gene product forms part of a complex with the glucocorticoid receptor and can modulate cortisol-binding affinity. Variations in the gene have been associated with increased recurrence of depression and with rapid response to antidepressant treatment. We sought to determine whether common FKBP5 variants confer risk for bipolar disorder. We genotyped seven tag single-nucleotide polymorphisms (SNPs) in FKBP5, plus two SNPs previously associated with illness, in 317 families with 554 bipolar offspring, derived primarily from two studies. Single marker and haplotypic analyses were carried out with FBAT and EATDT employing the standard bipolar phenotype. Association analyses were also conducted using 11 disease-related variables as covariates. Under an additive genetic model, rs4713902 showed significant overtransmission of the major allele (P=0.0001), which was consistent across the two sample sets (P=0.004 and 0.006). rs7757037 showed evidence of association that was strongest under the dominant model (P=0.001). This result was consistent across the two datasets (P=0.017 and 0.019). The dominant model yielded modest evidence for association (P<0.05) for three additional markers. Covariate-based analyses suggested that genetic variation within FKBP5 may influence attempted suicide and number of depressive episodes in bipolar subjects. Our results are consistent with the well-established relationship between the hypothalamic-pituitary-adrenal (HPA) axis, which mediates the stress response through regulation of cortisol, and mood disorders. Ongoing whole-genome association studies in bipolar disorder and major depression should further clarify the role of FKBP5 and other HPA genes in these illnesses.

KW - HPA axis

KW - Linkage disequilibrium

KW - Mood disorder

UR - http://www.scopus.com/inward/record.url?scp=60549096097&partnerID=8YFLogxK

U2 - 10.1038/sj.mp.4002141

DO - 10.1038/sj.mp.4002141

M3 - Article

C2 - 18180755

AN - SCOPUS:60549096097

SN - 1359-4184

VL - 14

SP - 261

EP - 268

JO - Molecular Psychiatry

JF - Molecular Psychiatry

IS - 3

ER -

Family-based association of FKBP5 in bipolar disorder

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