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利用连锁不平衡来确定6q14-q15上萨勒病基因座的精确遗传位置。

Linkage disequilibrium utilized to establish a refined genetic position of the Salla disease locus on 6q14-q15.

作者信息

Schleutker J, Laine A P, Haataja L, Renlund M, Weissenbach J, Aula P, Peltonen L

机构信息

Department of Medical Genetics, University of Turku, Finland.

出版信息

Genomics. 1995 May 20;27(2):286-92. doi: 10.1006/geno.1995.1044.

Abstract

Salla disease (SD), an inherited free sialic acid storage disorder, is caused by impaired transport of free sialic acid across the lysosomal membrane. Clinical characteristics of the disease include severe psychomotor retardation and some neurological abnormalities. We report here detailed linkage analyses of 50 Finnish SD families that localize the SD disease gene to a refined chromosomal area on 6q14-q15. The highest lod score of 17.30 was obtained with a microsatellite marker of locus D6S280. When linkage disequilibrium was adopted in the linkage analyses, we could further assign the SD locus to the immediate vicinity of marker locus D6S406. Linkage disequilibrium facilitated further restriction of the critical chromosomal region to approximately 80 kb, well within the limits of positional cloning techniques.

摘要

唾液酸贮积症(SD)是一种遗传性游离唾液酸贮积障碍疾病,由游离唾液酸跨溶酶体膜转运受损所致。该疾病的临床特征包括严重的精神运动发育迟缓及一些神经学异常表现。我们在此报告对50个芬兰SD家系进行的详细连锁分析,这些分析将SD疾病基因定位到6号染色体14 - 15区一个精细的染色体区域。使用位点D6S280的微卫星标记获得了最高连锁对数分值17.30。当在连锁分析中采用连锁不平衡时,我们能够进一步将SD基因座定位到标记位点D6S406紧邻区域。连锁不平衡有助于将关键染色体区域进一步限定至约80 kb,这完全在定位克隆技术的范围内。

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