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人类CYP51A1的核苷酸变异性较低:胆固醇和胆汁酸合成以及外源性物质代谢途径的荟萃分析

Low nucleotide variability of CYP51A1 in humans: meta-analysis of cholesterol and bile acid synthesis and xenobiotic metabolism pathways.

作者信息

Lewiñska Monika, Zmrzljak Ursula Prosenc, Rozman Damjana

出版信息

Acta Chim Slov. 2013;60(4):875-83.

Abstract

Lanosterol 14a-demethylase CYP51 is the most conserved cytochrome P450 (CYP) and is a part of hepatic cholesterol synthesis. Other liver CYPs contribute to cholesterol detoxification through bile acids or to xenobiotic detoxification (DM). To get novel insights into characteristics of the CYP51A1 locus that was so far not linked to human disorders we performed a meta-analysis of CYP51A1 gene polymorphisms in comparison to other liver CYPs and other genes of cholesterol synthesis. Cholesterol linked genes are generally less polymorphic than DM CYPs, with less coding variants, indicating differences in selection pressure between cholesterol and xenobiotic pathways. Among the studied liver CYPs, CYP51A1 has the lowest number of coding variants, and less common variants compared to average for cholesterol synthesis. We were not able to detect other functional molecules within the CYP51 gene (such as lincRNA or miRNA), so we looked into the entire gene locus. We found the AL133568 sequence that overlaps with the CYP51A1 promoter region. Our hypothesis was that the AL133568 transcript may have a role in regulating CYP51A1 expression, but we were unable to prove this experimentally. The reason for the low population variability of the human CYP51A1 thus remains uncertain.

摘要

羊毛甾醇14α-脱甲基酶CYP51是最保守的细胞色素P450(CYP),是肝脏胆固醇合成的一部分。其他肝脏CYP通过胆汁酸参与胆固醇解毒或参与外源性物质解毒(药物代谢)。为了深入了解迄今为止尚未与人类疾病相关联的CYP51A1基因座的特征,我们对CYP51A1基因多态性与其他肝脏CYP以及胆固醇合成的其他基因进行了荟萃分析。与药物代谢CYP相比,与胆固醇相关的基因通常多态性较低,编码变异较少,这表明胆固醇和外源性物质代谢途径之间的选择压力存在差异。在所研究的肝脏CYP中,CYP51A1的编码变异数量最少,与胆固醇合成的平均水平相比,罕见变异也较少。我们未能在CYP51基因内检测到其他功能分子(如长链非编码RNA或微小RNA),因此我们研究了整个基因座。我们发现了与CYP51A1启动子区域重叠的AL133568序列。我们的假设是AL133568转录本可能在调节CYP51A1表达中起作用,但我们无法通过实验证明这一点。因此,人类CYP51A1低群体变异性的原因仍然不确定。

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