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针对胰岛素依赖型糖尿病易感性的人类基因组第二代筛查。

A second-generation screen of the human genome for susceptibility to insulin-dependent diabetes mellitus.

作者信息

Concannon P, Gogolin-Ewens K J, Hinds D A, Wapelhorst B, Morrison V A, Stirling B, Mitra M, Farmer J, Williams S R, Cox N J, Bell G I, Risch N, Spielman R S

机构信息

Virginia Mason Research Center, Seattle, Washington 98101, USA.

出版信息

Nat Genet. 1998 Jul;19(3):292-6. doi: 10.1038/985.

Abstract

During the past decade, the genetics of type 1 (insulin-dependent) diabetes mellitus (IDDM) has been studied extensively and the disorder has become a paradigm for genetically complex diseases. Previous genome screens and studies focused on candidate genes have provided evidence for genetic linkage between polymorphic DNA markers and 15 putative IDDM susceptibility loci, designated IDDM1-IDDM15. We have carried out a second-generation screen of the genome for linkage and analysed the data by multipoint linkage methods. An initial panel of 212 affected sibpairs (ASPs) was genotyped for 438 markers spanning all autosomes, and an additional 467 ASPs were used for follow-up genotyping. Other than the well-established linkage with the HLA region at chromosome 6p21.3, there was only one region, located on chromosome 1q and not previously reported, where the log likelihood ratio (lod) was greater than 3. Lods between 1.0 and 1.8 were found in six other regions, three of which have been reported in other studies. Another reported region, on chromosome 6q and loosely linked to HLA, also had an elevated lod. Little or no support was found for most reported IDDM loci (lods were less than 1), despite larger sample sizes in the present study.

摘要

在过去十年中,1型(胰岛素依赖型)糖尿病(IDDM)的遗传学得到了广泛研究,该疾病已成为遗传复杂疾病的范例。先前的全基因组筛查和针对候选基因的研究为多态性DNA标记与15个假定的IDDM易感基因座(命名为IDDM1-IDDM15)之间的遗传连锁提供了证据。我们进行了第二代全基因组连锁筛查,并通过多点连锁方法分析了数据。最初的一组212对患病同胞对(ASP)针对覆盖所有常染色体的438个标记进行了基因分型,另外467对ASP用于后续基因分型。除了与6号染色体p21.3处的HLA区域已确立的连锁关系外,仅在1号染色体上有一个先前未报道的区域,其对数似然比(lod)大于3。在其他六个区域发现lod值在1.0至1.8之间,其中三个区域在其他研究中已有报道。另一个报道的位于6号染色体q上且与HLA松散连锁的区域,其lod值也有所升高。尽管本研究样本量更大,但大多数报道的IDDM基因座几乎没有或没有得到支持(lod值小于1)。

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