Carrera de Biología, Facultad de Ciencias Biológicas, Universidad Central del Ecuador, Quito, Ecuador.
Unidad de Cuidados Críticos de Adultos, Hospital Quito Sur del Instituto Ecuatoriano de Securidad Social, Quito, Ecuador.
Front Cell Infect Microbiol. 2024 Apr 17;14:1322882. doi: 10.3389/fcimb.2024.1322882. eCollection 2024.
COVID-19 has a broad clinical spectrum, ranging from asymptomatic-mild form to severe phenotype. The severity of COVID-19 is a complex trait influenced by various genetic and environmental factors. Ethnic differences have been observed in relation to COVID-19 severity during the pandemic. It is currently unknown whether genetic variations may contribute to the increased risk of severity observed in Latin-American individuals The aim of this study is to investigate the potential correlation between gene variants at , , and genes and the severity of COVID-19 in a population from Quito, Ecuador. This observational case-control study was conducted at the Carrera de Biologia from the Universidad Central del Ecuador and the Hospital Quito Sur of the Instituto Ecuatoriano de Seguridad Social (Quito-SUR-IESS), Quito, Ecuador. Genotyping for gene variants at rs1024611 (A>G), rs10774671 (A>G), and rs10406145 (G>C) of , , and genes was performed on 100 COVID-19 patients (43 with severe form and 57 asymptomatic-mild) using RFLP-PCR. The genotype distribution of all SNVs throughout the entire sample of 100 individuals showed Hardy Weinberg equilibrium (=0.53, 0.35, and 0.4 for , , and , respectively). The HWE test did not find any statistically significant difference in genotype distribution between the study and control groups for any of the three SNVs. The multivariable logistic regression analysis showed that individuals with the GG of the rs1024611 gene variant had an increased association with the severe COVID-19 phenotype in a recessive model ( = 0.0003, OR = 6.43, 95% CI 2.19-18.89) and for the rs10774671 gene variant, the log-additive model showed a significant association with the severe phenotype of COVID-19 (=0.0084, OR=3.85, 95% CI 1.33-11.12). Analysis of haplotype frequencies revealed that the coexistence of GAG at , , and variants, respectively, in the same individual increased the presence of the severe COVID-19 phenotype (OR=2.273, 95% CI: 1.271-4.068, =0.005305). The findings of the current study suggests that the ethnic background affects the allele and genotype frequencies of genes associated with the severity of COVID-19. The experience with COVID-19 has provided an opportunity to identify an ethnicity-based approach to recognize genetically high-risk individuals in different populations for emerging diseases.
新型冠状病毒肺炎(COVID-19)具有广泛的临床谱,从轻症到重症不等。COVID-19 的严重程度是一种复杂的特征,受到多种遗传和环境因素的影响。在大流行期间,已经观察到 COVID-19 严重程度存在种族差异。目前尚不清楚遗传变异是否可能导致拉丁美洲个体中观察到的严重程度增加的风险。本研究的目的是探讨厄瓜多尔基多人群中 基因的 rs1024611(A>G)、rs10774671(A>G)和 rs10406145(G>C)基因变异与 COVID-19 严重程度之间的潜在相关性。这项观察性病例对照研究在厄瓜多尔基多的中央大学的生物学系和基多南方医院的厄瓜多尔社会保障研究所(Quito-SUR-IESS)进行。使用 RFLP-PCR 对 100 名 COVID-19 患者(43 名重症患者和 57 名无症状轻症患者)进行了 基因的 rs1024611(A>G)、rs10774671(A>G)和 rs10406145(G>C)基因变异的基因分型。在整个 100 人的样本中,所有 SNV 的基因型分布均显示 Hardy-Weinberg 平衡(=0.53、0.35 和 0.4,分别为 、和 )。HWE 检验未发现任何 SNV 在研究组和对照组之间的基因型分布存在统计学差异。多变量逻辑回归分析显示,在隐性模型中, 基因的 rs1024611 基因变异的 GG 个体与严重 COVID-19 表型呈正相关(=0.0003,OR=6.43,95%CI 2.19-18.89),对于 基因的 rs10774671 基因变异,对数加性模型显示与 COVID-19 的严重表型呈显著相关性(=0.0084,OR=3.85,95%CI 1.33-11.12)。单倍型频率分析表明,同一个体中 基因的 rs1024611、rs10774671 和 rs10406145 变异的 GAG 共存分别增加了严重 COVID-19 表型的存在(OR=2.273,95%CI:1.271-4.068,=0.005305)。本研究的结果表明,种族背景会影响与 COVID-19 严重程度相关的基因的等位基因和基因型频率。COVID-19 的经验为我们提供了一个机会,可以识别不同人群中与新兴疾病相关的基于种族的高风险个体。
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