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Genome‐wide scan in Portuguese Island families implicates multiple loci in bipolar disorder: Fine mapping adds support on chromosomes 6 and 11
Author(s) -
Pato Carlos N.,
Pato M.T.,
Kirby A.,
Petryshen T.L.,
Medeiros H.,
Carvalho C.,
Macedo A.,
Dourado A.,
Coelho I.,
Valente J.,
Soares M.J.,
Ferreira C.P.,
Lei M.,
Verner A.,
Hudson T.J.,
Morley C.P.,
Kennedy J.L.,
Azevedo M.H.,
Daly M.J.,
Sklar P.
Publication year - 2004
Publication title -
american journal of medical genetics part b: neuropsychiatric genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.393
H-Index - 126
eISSN - 1552-485X
pISSN - 1552-4841
DOI - 10.1002/ajmg.b.30001
Subject(s) - bipolar disorder , genome scan , locus (genetics) , genetics , hum , genome , gene mapping , biology , chromosome , genetic linkage , linkage (software) , allele , gene , microsatellite , art , cognition , neuroscience , performance art , art history
As part of an extensive study in the Portuguese Island population of families with multiple patients suffering from bipolar disorder and schizophrenia, we performed an initial genome‐wide scan of 16 extended families with bipolar disorder that identified three regions on chromosomes 2, 11, and 19 with genome‐wide suggestive linkage and several other regions, including chromosome 6q, also approached suggestive levels of significance. Dick et al. [2003: Am J Hum Genet 73:107–114] recently reported in a study of 250 families with bipolar disorder a maxLOD score of 3.61 near marker D6S1021 on chromosome 6q. This study replicates this finding having detected a peak NPL = 2.02 ( P = 0.025) with the same marker D6S1021(104.7 Mb). Higher‐density mapping provided additional support for loci on chromosome 6 including marker D6S1021 with an NPL = 2.59 ( P = 0.0068) and peaking at marker D6S1639 (125 Mb) with an NPL = 3.06 ( P = 0.0019). A similar pattern was detected with higher‐density mapping of chromosome 11 with an NPL = 3.15 ( P = 0.0014) at marker D11S1883 (63.1 Mb). Simulations at the density of our fine mapping data indicate that less than 1 scan out of 10 would find two such scores genome‐wide in the same scan by chance. Our findings provide additional support for a susceptibility locus for bipolar disorder on 6q, as well as, suggesting the importance of denser scans. Published 2004 Wiley‐Liss, Inc.