Evidence of susceptibility loci on 4q32 and 16p12 for bipolar disorder

doi:10.1093/hmg/ddg199

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Human Molecular Genetics, 2003, Vol. 12, No. 15 1907-1915
DOI: 10.1093/hmg/ddg199
© 2003 Oxford University Press

Evidence of susceptibility loci on 4q32 and 16p12 for bipolar disorder

Jenny M. Ekholm¹^,3, Tuula Kieseppä², Tero Hiekkalinna¹^,3, Timo Partonen², Tiina Paunio¹^,4, Markus Perola¹^,3, Jesper Ekelund¹^,2, Jouko Lönnqvist², Petra Pekkarinen-Ijäs¹^,2^,5 and Leena Peltonen¹^,3^,*

¹Department of Molecular Medicine and ²Department of Mental Health and Alcohol Research, National Public Health Institute, 00251 Helsinki, Finland, ³Department of Human Genetics, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095, USA, ⁴Department of Psychiatry, University of Helsinki, Helsinki, Finland and ⁵Department of Neurology, Helsinki University Central Hospital, Helsinki, Finland

Received March 26, 2003; Accepted June 3, 2003

We performed a genome-wide scan for susceptibility loci in bipolardisorder in a study sample colleted from the isolated Finnishpopulation, consisting of 41 families with at least two affectedsiblings. We identified one distinct locus on 16p12 providingsignificant evidence for linkage in two-point analysis (Z_max=3.4).Furthermore, three loci with a two-point LOD score >2.0 wereobserved with markers on 4q32, 12q23 and Xq25, the latter locushaving been earlier identified in one extended Finnish pedigree.In the second stage we fine mapped these chromosomal regionsand also genotyped additional family members. In the fine mappingstage, 4q32 provided significant evidence of linkage for thethree-point analyses (Z_max=3.6) and 16p12 produced a three-pointLOD score of 2.7. Since the identified chromosomal regions replicateearlier linkage findings in either bipolar disorder or othermental disorders, they should be considered good targets forfurther genetic analyses.

^* To whom correspondence should be addressed. Tel: +358 947448393;Fax: +358 947448480; Email: leena.peltonen{at}ktl.fi

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