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在I/LnJ小鼠中鉴定出与高密度脂蛋白胆固醇水平降低相关的X连锁甾醇-4-α-羧酸盐3-脱氢酶(Nsdhl)的一种新型多态性。

Identification of a novel polymorphism in X-linked sterol-4-alpha-carboxylate 3-dehydrogenase (Nsdhl) associated with reduced high-density lipoprotein cholesterol levels in I/LnJ mice.

作者信息

Bautz David J, Broman Karl W, Threadgill David W

机构信息

Department of Genetics, North Carolina State University, Raleigh, North Carolina 27695.

出版信息

G3 (Bethesda). 2013 Oct 3;3(10):1819-25. doi: 10.1534/g3.113.007567.

Abstract

Loci controlling plasma lipid concentrations were identified by performing a quantitative trait locus analysis on genotypes from 233 mice from a F2 cross between KK/HlJ and I/LnJ, two strains known to differ in their high-density lipoprotein (HDL) cholesterol levels. When fed a standard diet, HDL cholesterol concentration was affected by two significant loci, the Apoa2 locus on Chromosome (Chr) 1 and a novel locus on Chr X, along with one suggestive locus on Chr 6. Non-HDL concentration also was affected by loci on Chr 1 and X along with a suggestive locus on Chr 3. Additional loci that may be sex-specific were identified for HDL cholesterol on Chr 2, 3, and 4 and for non-HDL cholesterol on Chr 5, 7, and 14. Further investigation into the potential causative gene on Chr X for reduced HDL cholesterol levels revealed a novel, I/LnJ-specific nonsynonymous polymorphism in Nsdhl, which codes for sterol-4-alpha-carboxylate 3-dehydrogenase in the cholesterol synthesis pathway. Although many lipid quantitative trait locus have been reported previously, these data suggest there are additional genes left to be identified that control lipid levels and that can provide new pharmaceutical targets.

摘要

通过对KK/HlJ和I/LnJ这两个已知高密度脂蛋白(HDL)胆固醇水平存在差异的品系杂交产生的233只F2代小鼠的基因型进行数量性状基因座分析,确定了控制血浆脂质浓度的基因座。当喂食标准饮食时,HDL胆固醇浓度受两个显著基因座影响,即位于1号染色体(Chr)上的Apoa2基因座和X染色体上的一个新基因座,以及6号染色体上的一个提示性基因座。非HDL浓度也受1号和X号染色体上的基因座以及3号染色体上的一个提示性基因座影响。在2号、3号和4号染色体上发现了可能具有性别特异性的其他HDL胆固醇基因座,在5号、7号和14号染色体上发现了非HDL胆固醇基因座。对X染色体上导致HDL胆固醇水平降低的潜在致病基因的进一步研究揭示了Nsdhl基因中一种新的、I/LnJ特异性的非同义多态性,该基因在胆固醇合成途径中编码固醇-4-α-羧酸盐3-脱氢酶。尽管此前已报道了许多脂质数量性状基因座,但这些数据表明,仍有其他控制脂质水平的基因有待发现,这些基因可提供新的药物靶点。

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