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1型糖尿病中11号染色体q13区域LRP5基因座的连锁与关联定位

Linkage and association mapping of the LRP5 locus on chromosome 11q13 in type 1 diabetes.

作者信息

Twells Rebecca C J, Mein Charles A, Payne Felicity, Veijola Riitta, Gilbey Matthew, Bright Matthew, Timms Andrew, Nakagawa Yusuke, Snook Hywel, Nutland Sarah, Rance Helen E, Carr Philippa, Dudbridge Frank, Cordell Heather J, Cooper Jason, Tuomilehto-Wolf Eva, Tuomilehto Jaakko, Phillips Michael, Metzker Michael, Hess J Fred, Todd John A

机构信息

Department of Medical Genetics, JDRF/WT Diabetes and Inflammation Laboratory, Cambridge Institute for Medical Research, University of Cambridge, Wellcome Trust/MRC Building, Addenbrooke's Hospital, Cambridge CB2 2XY, UK.

出版信息

Hum Genet. 2003 Jul;113(2):99-105. doi: 10.1007/s00439-003-0940-6. Epub 2003 Apr 17.

Abstract

Linkage of chromosome 11q13 to type 1 diabetes (T1D) was first reported from genome scans (Davies et al. 1994; Hashimoto et al. 1994) resulting in P <2.2 x 10(-5) (Luo et al. 1996) and designated IDDM4 ( insulin dependent diabetes mellitus 4). Association mapping under the linkage peak using 12 polymorphic microsatellite markers suggested some evidence of association with a two-marker haplotype, D11S1917*03-H0570POLYA*02, which was under-transmitted to affected siblings and over-transmitted to unaffected siblings ( P=1.5 x 10(-6)) (Nakagawa et al. 1998). Others have reported evidence for T1D association of the microsatellite marker D11S987, which is approximately 100 kb proximal to D11S1917 (Eckenrode et al. 2000). We have sequenced a 400-kb interval surrounding these loci and identified four genes, including the low-density lipoprotein receptor related protein (LRP5) gene, which has been considered as a functional candidate gene for T1D (Hey et al. 1998; Twells et al. 2001). Consequently, we have developed a comprehensive SNP map of the LRP5 gene region, and identified 95 SNPs encompassing 269 kb of genomic DNA, characterised the LD in the region and haplotypes (Twells et al. 2003). Here, we present our refined linkage curve of the IDDM4 region, comprising 32 microsatellite markers and 12 SNPs, providing a peak MLS=2.58, P=5 x 10(-4), at LRP5 g.17646G>T. The disease association data, largely focused in the LRP5 region with 1,106 T1D families, provided no further evidence for disease association at LRP5 or at D11S987. A second dataset, comprising 1,569 families from Finland, failed to replicate our previous findings at LRP5. The continued search for the variants of the putative IDDM4 locus will greatly benefit from the future development of a haplotype map of the genome.

摘要

11号染色体q13与1型糖尿病(T1D)的连锁关系最早是在基因组扫描中报道的(戴维斯等人,1994年;桥本等人,1994年),得到的P值<2.2×10⁻⁵(罗等人,1996年),并被命名为IDDM4(胰岛素依赖型糖尿病4)。在连锁峰值下使用12个多态性微卫星标记进行关联图谱分析,提示了与一种双标记单倍型D11S1917*03 - H0570POLYA*02存在关联的一些证据,该单倍型向患病同胞的传递不足,向未患病同胞的传递过度(P = 1.5×10⁻⁶)(中川等人,1998年)。其他人报道了微卫星标记D11S987与T1D关联的证据,该标记位于D11S1917近端约100 kb处(埃肯罗德等人,2000年)。我们对这些基因座周围400 kb的区间进行了测序,鉴定出四个基因,包括低密度脂蛋白受体相关蛋白(LRP5)基因,该基因被认为是T1D的一个功能候选基因(海伊等人,1998年;特韦尔斯等人,2001年)。因此,我们绘制了LRP5基因区域的综合单核苷酸多态性(SNP)图谱,鉴定出95个涵盖269 kb基因组DNA的SNP,对该区域的连锁不平衡(LD)和单倍型进行了特征分析(特韦尔斯等人,2003年)。在此,我们展示了IDDM4区域的精细连锁曲线,包括32个微卫星标记和12个SNP,在LRP5基因g.17646G>T处提供了一个峰值MLS = 2.58,P = 5×10⁻⁴。在1106个T1D家系中主要聚焦于LRP5区域的疾病关联数据,未提供LRP5或D11S987与疾病关联的进一步证据。包含来自芬兰的1569个家系的第二个数据集未能重复我们之前在LRP5上的发现。对假定的IDDM4基因座变异的持续搜索将极大地受益于未来基因组单倍型图谱的发展。

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