卡塔尔人口对传染病的遗传易感性

M. Smatti, Y. Al-Sarraj, O. Albagha, H. Yassine
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引用次数: 0

摘要

背景:传染病占卡塔尔每年死亡人数的8%,因此对公共卫生构成重大挑战。有趣的是,病毒感染的传播和严重程度在个人和人群之间差别很大。最近的例子是SARS-CoV-2,它的范围从轻度/无症状到严重的呼吸综合征。此前有报道称,在结核病、流感和艾滋病毒中观察到,与免疫相关的基因多态性可以影响个体对感染的反应;然而,在IDs中探索因果宿主遗传变异的研究仍然有限,并且在人群纳入方面显着偏斜。事实上,卡塔尔人群对id的遗传易感性在很大程度上是未知的。目的:进行全面的遗传筛查,以调查卡塔尔人群中与各种感染相关的变异的存在和频率。方法:先前使用Illumina HiSeq X Ten1测序仪对18,000名QBB参与者进行了全基因组测序。对原始数据进行了初始数据处理和质量评估,并创建了变量调用文件(VCF)。我们被允许访问6218个测序样本的VCF文件。然后使用PLINK-1.9将遗传变异数据转换为PLINK文件格式。采用标准化的质量保证和质量控制(QA/QC)方法,在snp和样品水平上产生高质量和置信度。用于计算等位基因频率的最终文件包含6047名受试者。此外,提取GWAS目录中已有文献报道的与感染相关的snp列表,用于计算和比较卡塔尔人基因组中与其他人群相比的等位基因频率。结果:卡塔尔人群中感染相关snp的频率在大多数感染中明显较低。大多数变异(78%)在卡塔尔基因组中显示负折叠变化。所有变异中只有22%在卡塔尔人群中比其他人群更普遍。最显著的差异是与结核病和艾滋病相关的基因(分别为200-940倍和160-710倍)。结论:本研究报告了卡塔尔人群对IDs的总体易感性较低。尽管如此,这也可能表明存在未知的卡塔尔独有变体,因此,强调了未来GWAS进一步研究的必要性。
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Genetic Susceptibility to Infectious Diseases in the Qatari Population
Background: Infectious diseases (IDs) account for 8% of deaths annually in Qatar, and therefore, represent a significant challenge for public health. Interestingly, the spread and severity of viral infections vary considerably between individuals and populations. The most recent example is SARS-CoV-2, which ranges from mild/asymptomatic to a severe respiratory syndrome. It has been previously reported that polymorphisms in genes linked to immunity can influence individuals’ responses to infections as observed in tuberculosis, influenza, and HIV; however, studies exploring causal host genetic variants in IDs are still limited and dramatically skewed with regard to population inclusion. In fact, the genetic susceptibility to IDs in the Qatari population is largely unknown. Aim: To perform a comprehensive genetic screening to investigate the presence and frequency of variants previously associated with various infections in the Qatari population. Methods: Whole-genome sequencing was previously performed for 18,000 QBB participants using Illumina HiSeq X Ten1 sequencers. The initial data processing and quality assessment of the raw data has also been performed and variant calling files (VCF) were created. We were granted the access to the VCF files of 6,218 sequenced samples. The genetic variant data was then converted to PLINK file format using PLINK-1.9. Standardized quality-assurance and quality control (QA/QC) methods were followed to generate high quality and confidence on both SNPs and sample levels. The final file used for calculating allele frequency contained 6,047 subjects. Additionally, list of infections-related SNPs that were previously reported in the literature and deposited in GWAS catalog was extracted and used to calculate and compare the allelic frequency in the Qatari genomes compared to other populations. Results: The frequency of infections-related SNPs in the Qatari population was significantly lower for most infections. Most variants (78%) showed negative fold change in the Qatari genomes. Only 22% of all variants were more prevalent in Qatari population compared to others. The most significant differences were observed in genes related to TB and HIV (200-940 and 160-710 fold change, respectively). Conclusion: This study reports a lower susceptibility of the Qatari population to IDs in general. Nonetheless, this might also indicate the presence of unknown Qatari-unique variants and hence, highlights the need for further investigation in future GWAS.
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