Smyth C, Kalsi G, Curtis D, Brynjolfsson J, O'Neill J, Rifkin L, Moloney E, Murphy P, Petursson H, Gurling H
Department of Psychiatry, University College London Medical School, United Kingdon.
Genomics. 1997 Feb 1;39(3):271-8. doi: 10.1006/geno.1996.4486.
Following a report of a linkage study that yielded evidence for a susceptibility locus for bipolar affective disorder on the long arm of chromosome 21, we studied 23 multiply affected pedigrees collected from Iceland and the UK, using the markers PFKL, D21S171, and D21S49. Counting only bipolar cases as affected, a two-point LOD of 1.28 was obtained using D21S171 (theta = 0.01, alpha = 0.35), with three Icelandic families producing LODs of 0.63, 0.62, and 1.74 (all at theta = 0.0). Affected sib pair analysis demonstrated increased allele sharing at D21S171 (P = 0.001) when unipolar cases were also considered affected. The same set of pedigrees had previously been typed for a tyrosine hydroxylase gene (TH) polymorphism at 11p15 and had shown some moderate evidence for linkage. When information from TH and the 21q markers was combined in a two-locus admixture analysis, an overall admixture LOD of 3.87 was obtained using the bipolar affection model. Thus the data are compatible with the hypothesis that a locus at or near TH influences susceptibility in some pedigrees, while a locus near D21S171 is active in others. Similar analyses in other datasets should be carried out to confirm or refute our tentative finding.
在一项连锁研究报告显示21号染色体长臂上存在双相情感障碍易感基因座的证据之后,我们使用PFKL、D21S171和D21S49标记,对从冰岛和英国收集的23个多病例家系进行了研究。仅将双相情感障碍病例计为患病,使用D21S171(θ = 0.01,α = 0.35)获得了两点LOD值为1.28,三个冰岛家系的LOD值分别为0.63、0.62和1.74(均在θ = 0.0时)。当也将单相情感障碍病例计为患病时,受累同胞对分析显示D21S171处的等位基因共享增加(P = 0.001)。同一组家系先前已针对11p15处的酪氨酸羟化酶基因(TH)多态性进行分型,并显示出一些中等程度的连锁证据。当在双位点混合分析中结合TH和21q标记的信息时,使用双相情感障碍患病模型获得的总体混合LOD值为3.87。因此,这些数据与以下假设相符:在某些家系中,TH处或其附近的一个基因座影响易感性,而在其他家系中,D21S171附近的一个基因座起作用。应在其他数据集中进行类似分析,以证实或反驳我们的初步发现。
