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通过关联分析和连锁分析,支持18号染色体短臂上的一个位点赋予精神分裂症家族中功能性精神病易感性。

Support for a chromosome 18p locus conferring susceptibility to functional psychoses in families with schizophrenia, by association and linkage analysis.

作者信息

Schwab S G, Hallmayer J, Lerer B, Albus M, Borrmann M, Hönig S, Strauss M, Segman R, Lichtermann D, Knapp M, Trixler M, Maier W, Wildenauer D B

机构信息

Molecular Genetics Laboratory, Department of Psychiatry, University of Bon, Germany.

出版信息

Am J Hum Genet. 1998 Oct;63(4):1139-52. doi: 10.1086/302046.

Abstract

The action of antipsychotic drugs on dopamine receptors suggests that dopaminergic signal transmission may play a role in the development of schizophrenia. We tested eight candidate genes (coding for dopamine receptors, the dopamine transporter, and G-proteins) in 59 families from Germany and Israel, for association. A P value of .00055 (.0044 when corrected for the no. of markers tested) was obtained for the intronic CA-repeat marker G-olfalpha on chromosome 18p. The value decreased to .000088 (.0007) when nine sibs with recurrent unipolar depressive disorder were included. Linkage analysis using SSLP markers densely spaced around G-olfalpha yielded a maximum two-point LOD score of 3.1 for a marker 0.5 cM distal to G-olfalpha. Multipoint analysis under the assumption of heterogeneity supported this linkage-whether the affected pheotype was defined narrowly or broadly-as did nonparametric linkage (NPL). In 12 families with exclusively maternal transmission of the disease, the NPL value also supported linkage to this marker. In order to test for association/linkage disequilibrium in the presence of linkage, the sample was restricted to independent offspring. When this sample was combined with 65 additional simplex families (each of them comprising one schizophrenic offspring and his or her parents), the 124-bp allele of G-olfalpha was transmitted 47 times and was not transmitted 21 times (P=.009). These results suggest the existence, on chromosome 18p, of a potential susceptibility locus for functional psychoses.

摘要

抗精神病药物对多巴胺受体的作用表明,多巴胺能信号传递可能在精神分裂症的发病过程中起作用。我们在来自德国和以色列的59个家庭中测试了8个候选基因(编码多巴胺受体、多巴胺转运体和G蛋白),以寻找关联。在18号染色体短臂上的内含子CA重复标记G-olfalpha获得了P值为0.00055(经测试标记数量校正后为0.0044)。当纳入9名患有复发性单相抑郁症的同胞时,该值降至0.000088(0.0007)。使用紧密围绕G-olfalpha分布的SSLP标记进行连锁分析,对于位于G-olfalpha远端0.5 cM处的一个标记,获得了最大两点LOD分数为3.1。在假设存在异质性的情况下进行多点分析支持了这种连锁关系——无论受影响的表型是狭义定义还是广义定义——非参数连锁分析(NPL)也是如此。在12个疾病仅由母亲传递的家庭中,NPL值也支持与该标记的连锁关系。为了在存在连锁的情况下测试关联/连锁不平衡,样本仅限于独立后代。当将该样本与另外65个单系家庭(每个家庭包括一个精神分裂症后代及其父母)合并时,G-olfalpha的124-bp等位基因传递了47次,未传递21次(P = 0.009)。这些结果表明,在18号染色体短臂上存在一个功能性精神病的潜在易感基因座。

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