Initial genome scan of the NIMH genetics initiative bipolar pedigrees: Chromosomes 4, 7, 9, 18, 19, 20, and 21q

Sevilla D. Detera-Wadleigh; Judith A. Badner; Takeo Yoshikawa; Alan R. Sanders; Lynn R. Goldin; Gordon Turner; Denise Y. Rolling; Tracy Moses; Juliet J. Guroff; Diane Kazuba; Mary E. Maxwell; Howard J. Edenberg; Tatiana Foroud; Debomoy Lahiri; John I. Nurnberger; O. Colin Stine; Francis McMahon; Deborah A. Meyers; Dean MacKinnon; Sylvia Simpson; Melvin McInnis; J. Raymond DePaulo; John Rice; Alison Goate; Theodore Reich; Mary C. Blehar; Elliot S. Gershon

doi:10.1002/(SICI)1096-8628(19970531)74:3<254::AID-AJMG4>3.0.CO;2-Q

Initial genome scan of the NIMH genetics initiative bipolar pedigrees: Chromosomes 4, 7, 9, 18, 19, 20, and 21q

Sevilla D. Detera-Wadleigh, Judith A. Badner, Takeo Yoshikawa, Alan R. Sanders, Lynn R. Goldin, Gordon Turner, Denise Y. Rolling, Tracy Moses, Juliet J. Guroff, Diane Kazuba, Mary E. Maxwell, Howard J. Edenberg, Tatiana Foroud, Debomoy Lahiri, John I. Nurnberger, O. Colin Stine, Francis McMahon, Deborah A. Meyers, Dean MacKinnon, Sylvia SimpsonMelvin McInnis, J. Raymond DePaulo, John Rice, Alison Goate, Theodore Reich, Mary C. Blehar, Elliot S. Gershon

School of Medicine

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

115 Scopus citations

Abstract

An initial genome scan was performed on 540 individuals from 97 families segregating bipolar disorder, collected through the National Institutes of Mental Health Genetics Initiative. We report here affected-sib-pair (ASP) data on 126 marker loci (≃68,000 genotypes) mapping to chromosomes 4, 7, 9, 18, 19, 20, and 21q, under three affection status models. Modest increases in identical-by-descent (IBD) allele sharing were found at the following loci: D4S2397 and D4S391 (P < 0.05) on 4p, D4S1647 (P < 0.05) on 4q, D7S1802 and D7S1869 (low P = 0.01) on 7p, D9S302 (P = 0.004) on 9q, and D20S604 on 20p and D20S173 on 20q (P ≤ 0.05). In addition, five markers on 7q displayed increased IBD sharing (P = 0.046-0.002). Additional ASP analyses on chromosomes 18 and 21q marker data were performed using disease phenotype models defined previously. On chromosome 18, only D18S40 on 18p and D18S70 on 18q yielded a slight elevation in allele sharing (P = 0.02), implying that the reported linkages in these regions were not confirmed. On chromosome 21q, a cluster of markers within an ≃9 cM interval: D21S1254, D21S65, D21S1440, and D21S1255 exhibited excess allele sharing (P = 0.041-0.008). Multilocus data on overlapping marker quartets, from D21S1265 to D21S1255, which were consistent with increased IBD sharing (P < 0.01, with a low of 0.0009), overlapped a broad interval of excess allele sharing reported previously, increasing support for a susceptibility locus for bipolar disorder on 21q.

Original language	English (US)
Pages (from-to)	254-262
Number of pages	9
Journal	American Journal of Medical Genetics - Neuropsychiatric Genetics
Volume	74
Issue number	3
DOIs	https://doi.org/10.1002/(SICI)1096-8628(19970531)74:3<254::AID-AJMG4>3.0.CO;2-Q
State	Published - 1997

Keywords

Bipolar disorder
Bipolar pedigree
Genome scan
Linkage

ASJC Scopus subject areas

Genetics(clinical)
Psychiatry and Mental health
Cellular and Molecular Neuroscience

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10.1002/(SICI)1096-8628(19970531)74:3<254::AID-AJMG4>3.0.CO;2-Q

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Detera-Wadleigh, S. D., Badner, J. A., Yoshikawa, T., Sanders, A. R., Goldin, L. R., Turner, G., Rolling, D. Y., Moses, T., Guroff, J. J., Kazuba, D., Maxwell, M. E., Edenberg, H. J., Foroud, T., Lahiri, D., Nurnberger, J. I., Stine, O. C., McMahon, F., Meyers, D. A., MacKinnon, D., ... Gershon, E. S. (1997). Initial genome scan of the NIMH genetics initiative bipolar pedigrees: Chromosomes 4, 7, 9, 18, 19, 20, and 21q. American Journal of Medical Genetics - Neuropsychiatric Genetics, 74(3), 254-262. https://doi.org/10.1002/(SICI)1096-8628(19970531)74:3<254::AID-AJMG4>3.0.CO;2-Q

Detera-Wadleigh, SD, Badner, JA, Yoshikawa, T, Sanders, AR, Goldin, LR, Turner, G, Rolling, DY, Moses, T, Guroff, JJ, Kazuba, D, Maxwell, ME, Edenberg, HJ, Foroud, T, Lahiri, D, Nurnberger, JI, Stine, OC, McMahon, F, Meyers, DA, MacKinnon, D, Simpson, S, McInnis, M, DePaulo, JR, Rice, J, Goate, A, Reich, T, Blehar, MC & Gershon, ES 1997, 'Initial genome scan of the NIMH genetics initiative bipolar pedigrees: Chromosomes 4, 7, 9, 18, 19, 20, and 21q', American Journal of Medical Genetics - Neuropsychiatric Genetics, vol. 74, no. 3, pp. 254-262. https://doi.org/10.1002/(SICI)1096-8628(19970531)74:3<254::AID-AJMG4>3.0.CO;2-Q

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abstract = "An initial genome scan was performed on 540 individuals from 97 families segregating bipolar disorder, collected through the National Institutes of Mental Health Genetics Initiative. We report here affected-sib-pair (ASP) data on 126 marker loci (≃68,000 genotypes) mapping to chromosomes 4, 7, 9, 18, 19, 20, and 21q, under three affection status models. Modest increases in identical-by-descent (IBD) allele sharing were found at the following loci: D4S2397 and D4S391 (P < 0.05) on 4p, D4S1647 (P < 0.05) on 4q, D7S1802 and D7S1869 (low P = 0.01) on 7p, D9S302 (P = 0.004) on 9q, and D20S604 on 20p and D20S173 on 20q (P ≤ 0.05). In addition, five markers on 7q displayed increased IBD sharing (P = 0.046-0.002). Additional ASP analyses on chromosomes 18 and 21q marker data were performed using disease phenotype models defined previously. On chromosome 18, only D18S40 on 18p and D18S70 on 18q yielded a slight elevation in allele sharing (P = 0.02), implying that the reported linkages in these regions were not confirmed. On chromosome 21q, a cluster of markers within an ≃9 cM interval: D21S1254, D21S65, D21S1440, and D21S1255 exhibited excess allele sharing (P = 0.041-0.008). Multilocus data on overlapping marker quartets, from D21S1265 to D21S1255, which were consistent with increased IBD sharing (P < 0.01, with a low of 0.0009), overlapped a broad interval of excess allele sharing reported previously, increasing support for a susceptibility locus for bipolar disorder on 21q.",

keywords = "Bipolar disorder, Bipolar pedigree, Genome scan, Linkage",

author = "Detera-Wadleigh, {Sevilla D.} and Badner, {Judith A.} and Takeo Yoshikawa and Sanders, {Alan R.} and Goldin, {Lynn R.} and Gordon Turner and Rolling, {Denise Y.} and Tracy Moses and Guroff, {Juliet J.} and Diane Kazuba and Maxwell, {Mary E.} and Edenberg, {Howard J.} and Tatiana Foroud and Debomoy Lahiri and Nurnberger, {John I.} and Stine, {O. Colin} and Francis McMahon and Meyers, {Deborah A.} and Dean MacKinnon and Sylvia Simpson and Melvin McInnis and DePaulo, {J. Raymond} and John Rice and Alison Goate and Theodore Reich and Blehar, {Mary C.} and Gershon, {Elliot S.}",

year = "1997",

doi = "10.1002/(SICI)1096-8628(19970531)74:3<254::AID-AJMG4>3.0.CO;2-Q",

language = "English (US)",

volume = "74",

pages = "254--262",

journal = "American Journal of Medical Genetics - Neuropsychiatric Genetics",

issn = "1552-4841",

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number = "3",

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T1 - Initial genome scan of the NIMH genetics initiative bipolar pedigrees

T2 - Chromosomes 4, 7, 9, 18, 19, 20, and 21q

AU - Detera-Wadleigh, Sevilla D.

AU - Badner, Judith A.

AU - Yoshikawa, Takeo

AU - Sanders, Alan R.

AU - Goldin, Lynn R.

AU - Turner, Gordon

AU - Rolling, Denise Y.

AU - Moses, Tracy

AU - Guroff, Juliet J.

AU - Kazuba, Diane

AU - Maxwell, Mary E.

AU - Edenberg, Howard J.

AU - Foroud, Tatiana

AU - Lahiri, Debomoy

AU - Nurnberger, John I.

AU - Stine, O. Colin

AU - McMahon, Francis

AU - Meyers, Deborah A.

AU - MacKinnon, Dean

AU - Simpson, Sylvia

AU - McInnis, Melvin

AU - DePaulo, J. Raymond

AU - Rice, John

AU - Goate, Alison

AU - Reich, Theodore

AU - Blehar, Mary C.

AU - Gershon, Elliot S.

PY - 1997

Y1 - 1997

N2 - An initial genome scan was performed on 540 individuals from 97 families segregating bipolar disorder, collected through the National Institutes of Mental Health Genetics Initiative. We report here affected-sib-pair (ASP) data on 126 marker loci (≃68,000 genotypes) mapping to chromosomes 4, 7, 9, 18, 19, 20, and 21q, under three affection status models. Modest increases in identical-by-descent (IBD) allele sharing were found at the following loci: D4S2397 and D4S391 (P < 0.05) on 4p, D4S1647 (P < 0.05) on 4q, D7S1802 and D7S1869 (low P = 0.01) on 7p, D9S302 (P = 0.004) on 9q, and D20S604 on 20p and D20S173 on 20q (P ≤ 0.05). In addition, five markers on 7q displayed increased IBD sharing (P = 0.046-0.002). Additional ASP analyses on chromosomes 18 and 21q marker data were performed using disease phenotype models defined previously. On chromosome 18, only D18S40 on 18p and D18S70 on 18q yielded a slight elevation in allele sharing (P = 0.02), implying that the reported linkages in these regions were not confirmed. On chromosome 21q, a cluster of markers within an ≃9 cM interval: D21S1254, D21S65, D21S1440, and D21S1255 exhibited excess allele sharing (P = 0.041-0.008). Multilocus data on overlapping marker quartets, from D21S1265 to D21S1255, which were consistent with increased IBD sharing (P < 0.01, with a low of 0.0009), overlapped a broad interval of excess allele sharing reported previously, increasing support for a susceptibility locus for bipolar disorder on 21q.

AB - An initial genome scan was performed on 540 individuals from 97 families segregating bipolar disorder, collected through the National Institutes of Mental Health Genetics Initiative. We report here affected-sib-pair (ASP) data on 126 marker loci (≃68,000 genotypes) mapping to chromosomes 4, 7, 9, 18, 19, 20, and 21q, under three affection status models. Modest increases in identical-by-descent (IBD) allele sharing were found at the following loci: D4S2397 and D4S391 (P < 0.05) on 4p, D4S1647 (P < 0.05) on 4q, D7S1802 and D7S1869 (low P = 0.01) on 7p, D9S302 (P = 0.004) on 9q, and D20S604 on 20p and D20S173 on 20q (P ≤ 0.05). In addition, five markers on 7q displayed increased IBD sharing (P = 0.046-0.002). Additional ASP analyses on chromosomes 18 and 21q marker data were performed using disease phenotype models defined previously. On chromosome 18, only D18S40 on 18p and D18S70 on 18q yielded a slight elevation in allele sharing (P = 0.02), implying that the reported linkages in these regions were not confirmed. On chromosome 21q, a cluster of markers within an ≃9 cM interval: D21S1254, D21S65, D21S1440, and D21S1255 exhibited excess allele sharing (P = 0.041-0.008). Multilocus data on overlapping marker quartets, from D21S1265 to D21S1255, which were consistent with increased IBD sharing (P < 0.01, with a low of 0.0009), overlapped a broad interval of excess allele sharing reported previously, increasing support for a susceptibility locus for bipolar disorder on 21q.

KW - Bipolar disorder

KW - Bipolar pedigree

KW - Genome scan

KW - Linkage

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AN - SCOPUS:17744410079

SN - 1552-4841

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ER -

Initial genome scan of the NIMH genetics initiative bipolar pedigrees: Chromosomes 4, 7, 9, 18, 19, 20, and 21q

Abstract

Keywords

ASJC Scopus subject areas

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