Frequency of rs1051338 and rs116928232 Variants in Individuals from Northwest Mexico

IF 2.6 4区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY
Angélica Alejandra Hernández-Orozco, Lennon Melendez-Aranda, Sandra del Carmen Mendoza-Ruvalcaba, Francisco Javier Perea-Díaz, Jorge J. Cebolla, Pilar Giraldo, Aniel Jessica Leticia Brambila-Tapia, José Elías García-Ortíz
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引用次数: 0

Abstract

Background

LIPA, situated on chromosome 10q23.2-q23.3, encodes the enzyme lysosomal acid lipase (LAL) (EC 3.1.1.13). Genetic alterations in LIPA lead to lysosomal acid lipase deficiency (LALD), an inborn error causing lipid metabolism anomalies and impairing cholesterol and triacylglyceride degradation. Over 40 LIPA variants have been documented, yet this study focuses on just two. The rs1051338 variant (NM_000235:c.46A>C) affects the signal peptide in Exon 2, whereas rs116928232, located in Exon 8, alters the splice site (NM_000235:c.894G>A), impacting lysosomal acid lipase activity. Considering the diverse clinical manifestations of LALD and the rising hepatic steatosis prevalence in Mexican population, mainly due to diet, these variants were investigated within this demographic to uncover potential contributing factors. This study aimed to reveal the frequency of rs1051338 and rs116928232 among healthy mestizo individuals in Northwest Mexico, marking a significant genetic exploration in this demographic.

Methods

Three hundred ten healthy mestizo individuals underwent PCR-RFLP analysis for both variants, and Sanger sequencing was performed for variant rs116928232. Bioinformatic analysis was also performed to predict protein changes.

Results

Allele frequencies for rs1051338 (FA = 0.39, p value = 0.15) and rs116928232 (FA = 0.0016, p value = 0.49) aligned with reported data, while bioinformatic analysis allowed us to identify the protein alteration observed in both variants; finally, the variants showed no linkage between them (normalized D′ = 1.03, p value = 0.56).

Conclusions

Allelic frequencies closely matched reported data, and protein structure analysis confirmed variant impacts on LAL enzyme function. Notably, this study marks the first analysis of rs1051338 and rs116928232 in a healthy Mexican mestizo population.

Abstract Image

墨西哥西北部个体中 rs1051338 和 rs116928232 变异的频率。
背景:LIPA位于染色体10q23.2-q23.3上,编码溶酶体酸性脂肪酶(LAL)(EC 3.1.1.13)。LIPA 基因的改变会导致溶酶体酸性脂肪酶缺乏症(LALD),这是一种先天性疾病,会导致脂质代谢异常,影响胆固醇和三酰甘油的降解。已有 40 多个 LIPA 变异被记录在案,但本研究只关注其中的两个。rs1051338 变体(NM_000235:c.46A>C)影响外显子 2 中的信号肽,而位于外显子 8 中的 rs116928232 则改变了剪接位点(NM_000235:c.894G>A),从而影响溶酶体酸性脂肪酶的活性。考虑到 LALD 的临床表现多种多样,而且主要由于饮食习惯,墨西哥人的肝脂肪变性发病率不断上升,因此在这一人群中对这些变异进行了调查,以发现潜在的诱因。本研究旨在揭示 rs1051338 和 rs116928232 在墨西哥西北部健康混血人群中的频率,这标志着在该人群中进行了一次重要的遗传学探索:方法: 对 3100 名健康的混血人进行了这两个变异体的 PCR-RFLP 分析,并对变异体 rs116928232 进行了 Sanger 测序。此外,还进行了生物信息学分析,以预测蛋白质的变化:结果:rs1051338(FA = 0.39,p 值 = 0.15)和 rs116928232(FA = 0.0016,p 值 = 0.49)的等位基因频率与报告数据一致,而生物信息分析使我们能够确定在这两个变异体中观察到的蛋白质变化;最后,这两个变异体之间没有关联(归一化 D' = 1.03,p 值 = 0.56):结论:等位基因频率与报道的数据非常吻合,蛋白质结构分析证实了变体对 LAL 酶功能的影响。值得注意的是,本研究是首次在墨西哥混血健康人群中对 rs1051338 和 rs116928232 进行分析。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Clinical Laboratory Analysis
Journal of Clinical Laboratory Analysis 医学-医学实验技术
CiteScore
5.60
自引率
7.40%
发文量
584
审稿时长
6-12 weeks
期刊介绍: Journal of Clinical Laboratory Analysis publishes original articles on newly developing modes of technology and laboratory assays, with emphasis on their application in current and future clinical laboratory testing. This includes reports from the following fields: immunochemistry and toxicology, hematology and hematopathology, immunopathology, molecular diagnostics, microbiology, genetic testing, immunohematology, and clinical chemistry.
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