Authors
Ophoff, Roel A.
Escamilla, Michael A.
Service, Susan K.
Spesny, Mitzi
Gallegos, Alvaro
Mathews, Carol
Neylan, Thomas
Batki, Steven L.
Roche, Erin
Ramirez, Margarita
Silva, Sandra
De Mille, Melissa C.
Dong, Penny
Leon, Pedro E.
Reus, Victor I.
Sandkuijl, Lodewijk A.
Freimer, Nelson B.
Meshi, Dar B.
Poon, Wingman
Molina, Julio
Citation
A. Ophoff, Roel et al., Genomewide Linkage Disequilibrium Mapping of Severe Bipolar Disorder in a Population Isolate, American journal of human genetics , 71(3), 2002, pp. 565-574
Journal title
ISSN journal
00029297
Volume
71
Issue
3
Year of publication
2002
Pages
565 - 574
Database
ACNP
SICI code
Abstract
Genomewide association studies may offer the best promise for genetic mapping of complex traits. Such studies in outbred populations require very densely spaced single-nucleotide polymorphisms. In recently founded population isolates, however, extensive linkage disequilibrium (LD) may make these studies feasible with currently available sets of short tandem repeat markers, spaced at intervals as large as a few centimorgans. We report the results of a genomewide association study of severe bipolar disorder (BP-I), using patients from the isolated population of the central valley of Costa Rica. We observed LD with BP-I on several chromosomes; the most striking results were in proximal 8p, a region that has previously shown linkage to schizophrenia. This region could be important for severe psychiatric disorders, rather than for a specific phenotype.