肥胖与瘦素受体基因多态性的儿童。

Q3 Medicine
Aleksandr Abaturov, Anna Nikulina
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引用次数: 4

摘要

基于下一代基因组测序(NGS)数据的瘦素受体基因(LEPR)单核苷酸多态性(snp)研究正成为代谢健康(MHO)和代谢不健康肥胖(MUO)表型诊断、治疗和预防的一个越来越重要的方面。材料与方法:采用NGS法结合生物信息学分析对35例6 ~ 18岁的肥胖儿童进行检查。根据国家心肺血液研究所专家组的建议,主要组(n = 18)由MUO患儿组成。对照组(n = 17)为MHO患儿。统计方法:方差分析、Wald序贯分析、Spearman相关分析、名义数据分析、多元判别分析。结果:已鉴定出肥胖儿童LEPR基因的10种非同义性snp (rs3790435、rs1137100、rs2186248、rs70940803、rs79639154、rs1359482195、rs1137101、rs1805094、rs13306520、rs13306522)。多重判别分析表明,以下几个LEPR snp在MUO的发展中最为重要:rs3790435、rs13306522、rs13306520。标称数据分析显示,LEPR基因拷贝数变异(Copy number variation, CNV) rs3790435组间差异显著。Wald's分析使我们确定了6个重要的MUO预测因子(І≥0.5):2 CNV rs3790435(相对风险,RR = 2,预后系数,PC = +2.76);男童(RR = 1.3, PC = +1.35);rs3790435 (RR = 1.9, PC = +2.76);高瘦素血症> 40.56 ng/ml (RR = 2, PC = +3);CNV rs1359482195≥3 (RR = 1.9, PC = +5.8);LEPR基因SNP≥4 (RR = 3.8, PC = +5.8)。结论:rs3790435基因型LEPR患儿更易发生MUO。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Obesity in Children with Leptin Receptor Gene Polymorphisms.

Introduction: The study of single nucleotide polymorphisms (SNPs) of the leptin receptor gene (LEPR) based on next generation genomic sequencing (NGS) data is becoming an increasingly important aspect of diagnosis, treatment and prevention of both metabolically healthy (MHO) and metabolically unhealthy obesity (MUO) phenotypes.

Material and methods: 35 obese children 6-18 years old were examined by the NGS method with bioinformatic analysis. The main group (n = 18) was formed by children with MUO, according to the recommendations of the expert group of the National Heart, Lung, and Blood Institute. The control group (n = 17) was represented by children with MHO. Statistical methods were used: analysis of variance, Wald's sequential analysis, Spearman's correlation analysis, analysis of nominal data and multiple discriminant analysis.

Results: 10 types of non-synonymous SNPs (rs3790435, rs1137100, rs2186248, rs70940803, rs79639154, rs1359482195, rs1137101, rs1805094, rs13306520, rs13306522) of the LEPR gene in obese children have been identified. Multiple discriminant analysis demonstrated that the following LEPR SNPs are of greatest importance in the development of MUO: rs3790435, rs13306522, rs13306520. Analysis of nominal data revealed significant differences in the groups for Copy number variation (CNV) rs3790435 of the LEPR gene. Wald's analysis allowed us to identify 6 important predictors of MUO (І ≥ 0.5): 2 CNV rs3790435 (Relative Risk, RR = 2, Prognostic coefficient, PC = +2.76); male gender of the child (RR = 1.3, PC = +1.35); rs3790435 (RR = 1.9, PC = +2.76); hyperleptinemia more than 40.56 ng/ml (RR = 2, PC = +3); CNV rs1359482195 ≥ 3 (RR = 1.9, PC = +5.8); SNP of the LEPR gene ≥4 (RR = 3.8, PC = +5.8).

Conclusion: Children with the genotype rs3790435 gene LEPR had signs of MUO more often.

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来源期刊
Acta medica (Hradec Kralove)
Acta medica (Hradec Kralove) Medicine-Medicine (all)
CiteScore
1.10
自引率
0.00%
发文量
8
审稿时长
20 weeks
期刊介绍: Acta Medica (Hradec Králové) is a multidisciplinary medical journal published by the Faculty of Medicine in Hradec Králové - Karolinum Press, the publishing house of Charles University. The journal is peer-reviewed and published quarterly in both paper and electronic form. The language of Acta Medica is English. Offerings include review articles, original articles, brief communications, case reports, announcements and notices. The journal was founded in 1958 under the title "A Collection of Scientific Works of the Charles University Faculty of Medicine in Hradec Kralove."
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