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魁北克东部人群的6p24 - 22区域与主要精神疾病。IREP研究小组。

6p24-22 region and major psychoses in the Eastern Quebec population. Le Groupe IREP.

作者信息

Maziade M, Bissonnette L, Rouillard E, Martinez M, Turgeon M, Charron L, Pouliot V, Boutin P, Cliche D, Dion C, Fournier J P, Garneau Y, Lavallée J C, Montgrain N, Nicole L, Pirès A, Ponton A M, Potvin A, Wallot H, Roy M A, Mérette C

机构信息

Centre de Recherche Université Laval Robert-Giffard, Beauport, Quebec,Canada.

出版信息

Am J Med Genet. 1997 May 31;74(3):311-8.

PMID:9184316
Abstract

Recent reports of a linkage trend in 6p24-22 for schizophrenia (SZ), in different samples, were tempered by the concurrent evidence of negative reports in other samples. In the studies showing positive results, different definitions of affection and a wide spectrum of diagnoses were used. Our objectives were not only to test for linkage at 6p24-22 in the Eastern Quebec population, but also to test whether this putative vulnerability locus was either selectively linked to schizophrenia (SZ), or to bipolar disorder (BP), or to both major psychoses. Parametric and nonparametric linkage analyses with 12 microsatellite markers in 6p24-p22 were performed on a sample of 18 large multigenerational pedigrees (N = 354) either affected by SZ, or by BP, or equally affected by both major psychoses (i.e., mixed pedigrees). Three affection definitions were usually tested in our program: one on schizophrenia (SZ), one on bipolar disorder (BP), and one that comprised SZ and BP under the hypothesis of a susceptibility locus common to both in major psychoses (common locus, CL). The results of parametric analyses did not support a major gene hypothesis. However, in one large mixed pedigree (#151), we observed with the common locus phenotype (CL) lod scores of 2.49 and 2.15, respectively, at the D6S296 and D6S277 loci under a dominant model. Our data suggest the presence of a potential vulnerability locus at 6p24-22 that could be related to both schizophrenia and bipolar affective disorder. These results may be seen as congruent with former studies that used schizoaffective as well as schizophrenia diagnoses as entry criteria for the affected families, and used an affection definition that comprised affective psychoses as well as schizophrenia.

摘要

最近在不同样本中报道了精神分裂症(SZ)与6p24 - 22区域存在连锁趋势,但同时其他样本中的阴性报道证据对此起到了缓和作用。在显示阳性结果的研究中,使用了不同的患病定义以及广泛的诊断范围。我们的目标不仅是在魁北克东部人群中检测6p24 - 22区域的连锁情况,还要测试这个假定的易患位点是选择性地与精神分裂症(SZ)、双相情感障碍(BP)相关,还是与这两种主要精神病都相关。我们对18个大型多代家系(N = 354)的样本进行了6p24 - p22区域12个微卫星标记的参数和非参数连锁分析,这些家系要么患有精神分裂症(SZ),要么患有双相情感障碍(BP),要么同时患有这两种主要精神病(即混合家系)。我们的程序通常测试三种患病定义:一种针对精神分裂症(SZ),一种针对双相情感障碍(BP),还有一种是在主要精神病中两者存在共同易感位点的假设下,将精神分裂症和双相情感障碍都纳入其中(共同位点,CL)。参数分析结果不支持主要基因假说。然而,在一个大型混合家系(#151)中,在显性模型下,我们在D6S296和D6S277位点观察到共同位点表型(CL)的对数优势分数分别为2.49和2.15。我们的数据表明在6p24 - 22区域存在一个潜在的易患位点,可能与精神分裂症和双相情感障碍都相关。这些结果可能与以前的研究一致,以前的研究将精神分裂症样情感障碍以及精神分裂症诊断作为受影响家庭的纳入标准,并使用了包括情感性精神病和精神分裂症的患病定义。

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