A genome-wide scan for linkage to chromosomal regions in 382 sibling pairs with schizophrenia or schizoaffective disorder
Author
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DeLisi, Lynn E.
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Shaw, Sarah H.
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Crow, Timothy J.
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Shields, Gail
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Smith, Angela B.
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Larach, Veronica W.
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Wellman, Nigel
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Loftus, Josephine
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Nanthakumar, Betsy
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Razi, Kamran
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Stewart, John
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Comazzi, Margherita
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Vita, Antonio
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Heffner, Thomas
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Sherrington, Robin
Admission date
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2019-01-29T17:51:07Z
Available date
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2019-01-29T17:51:07Z
Publication date
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2002
Cita de ítem
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American Journal of Psychiatry, Volumen 159, Issue 5, 2018, Pages 803-812
Identifier
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0002953X
Identifier
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10.1176/appi.ajp.159.5.803
Identifier
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https://repositorio.uchile.cl/handle/2250/163507
Abstract
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Objective: Some genome-wide scans and association studies for schizophrenia susceptibility genes have yielded significant positive findings, but there is disagreement between studies on their locations, and no mutation has yet been found in any gene. Since schizophrenia is a complex disorder, a study with sufficient power to detect a locus with a small or moderate gene effect is necessary. Method: In a genome-wide scan of 382 sibling pairs with a diagnosis of schizophrenia or schizoaffective disorder, 396 highly polymorphic markers spaced approximately 10 centimorgans apart throughout the genome were genotyped in all individuals. Multipoint nonparametric linkage analysis was performed to evaluate regions of the genome demonstrating increased allele sharing, as measured by a lod score. Results: Two regions with multipoint maximum lod scores suggesting linkage were found. The highest lod scores occurred on chromosome 10p15-p13 (peak lod score of 3.60 at marker D10S189) and the centromeri