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Author
Freedman, RobertLeonard, Sherry
Olincy, Ann
Kaufmann, Charles A.
Malaspina, Dolores
Cloninger, C. Robert
Svrakic, Dragan
Faraone, Stephen V.
Tsuang, Ming T.
Keyword
Genetics(clinical)schizophrenia; bipolar disorder; genetics; linkage analysis; chromosomes human pair 6, 10, and 15
Journal title
American Journal of Medical GeneticsDate Published
2002-08-21Publication Volume
105Publication Issue
8Publication Begin page
794Publication End page
800
Metadata
Show full item recordAbstract
Schizophrenia is assumed to have complex inheritance because of its high prevalence and sporadic familial transmission. Findings of linkage on different chromosomes in various studies corroborate this assumption. It is not known whether these ®endings represent heterogeneous inheritance, in which various ethnic groups inherit illness through different major gene effects, or multigenic inheritance, in which affected individuals inherit several common genetic abnormalities. This study therefore examined inheritance of schizophrenia at different genetic loci in a nationally collected European American and African American sample. Seventy-seven families were previously genotyped at 458 markers for the NIMH Schizophrenia Genetics Initiative. Initial genetic analysis tested a dominant model, with schizophrenia and schizoaffective disorder, depressed type, as the affected phenotype. The families showed one genome-wide significant linkage (Z ¼ 3.97) at chromosome 15q14, which maps within 1 cM of a previous linkage at the a7-nicotinic receptor gene. Chromosome 10p13 showed suggestive linkage (Z ¼ 2.40). Six others (6q21, 9q32, 13q32, 15q24, 17p12, 20q13) were positive, with few differences between the two ethnic groups. The probability of each family transmitting schizophrenia through two genes is greater than expected from the combination of the independent segregation of each gene. Two trait-locus linkage analysis supports a model in which genetic alleles associated with schizophrenia are relatively common in the general population and affected individuals inherit risk for illness through at least two different loci.DOI
10.1002/ajmg.10100ae974a485f413a2113503eed53cd6c53
10.1002/ajmg.10100
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