采用基于分子倒置探针(MIP)的 panel 测序分析中国原发性开角型青光眼个体的变异。
Analysis of variants in Chinese individuals with primary open-angle glaucoma using molecular inversion probe (MIP)-based panel sequencing.
机构信息
Department of ophthalmology, Daping Hospital of the Army Medical University, Chongqing, China.
Radiation & Cancer Biology Laboratory, Oncology Radiotherapy Center, Chongqing University Cancer Hospital & Chongqing Cancer Institute & Chongqing Cancer Hospital, Chongqing, China.
出版信息
Mol Vis. 2020 May 21;26:378-391. eCollection 2020.
PURPOSE
Family-based genetic linkage analysis and genome-wide association studies (GWASs) have identified many genomic loci associated with primary open-angle glaucoma (POAG). Several causative genes of POAG have been intensively analyzed by sequencing in different populations. However, few investigations have been conducted on the identification of variants of coding region in the genes identified in GWASs. Therefore, further research is needed to investigate whether they harbor pathogenically relevant rare coding variants and account for the observed association.
METHODS
To identify the potentially disease-relevant variants (PDVs) in POAG-associated genes in Chinese patients, we applied molecular inversion probe (MIP)-based panel sequencing to analyze 26 candidate genes in 235 patients with POAG and 241 control subjects.
RESULTS
The analysis identified 82 PDVs in 66 individuals across 235 patients with POAG. By comparison, only 18 PDVs in 19 control subjects were found, indicating an enrichment of PDVs in the POAG cohort (28.1% versus 7.9%, p = 8.629e-09). Among 26 candidate genes, the prevalence rate of PDVs in five genes showed a statistically significant difference between patients and controls (33 out of 235 versus 1 out of 241, p = 4.533e-10), including (p = 0.0033), (p = 0.0190), (p = 0.0140), (p = 0.0140), and (p = 0.0287). Furthermore, two sisters harboring a stop-loss mutation p.Ter494Glu were found in the POAG cohort, and further analysis of the family strongly suggested that p.Ter494Glu was a potentially disease-causing mutation for POAG. A statistically significant difference in age at diagnosis between patients with PDVs and those without PDVs was found, implying that some of the identified PDVs may have a role in promoting the early onset of POAG disease.
CONCLUSIONS
The results suggest that some of the associations identified in POAG risk loci can be ascribed to rare coding variants with likely functional effects that modify POAG risk.
目的
基于家系的遗传连锁分析和全基因组关联研究(GWAS)已经确定了许多与原发性开角型青光眼(POAG)相关的基因组位点。已经在不同人群中通过测序对 POAG 的几个致病基因进行了深入分析。然而,对于 GWAS 中鉴定的编码区变异的研究还很少。因此,需要进一步研究这些变异是否携带致病性相关的罕见编码变异,并解释观察到的关联。
方法
为了在 POAG 相关基因中鉴定与疾病相关的潜在变异(PDVs),我们应用基于分子倒置探针(MIP)的panel 测序对 235 名 POAG 患者和 241 名对照的 26 个候选基因进行了分析。
结果
在 235 名 POAG 患者的 66 名个体中鉴定出 82 个 PDVs。相比之下,在 19 名对照中仅发现 18 个 PDVs,表明 POAG 队列中 PDVs 富集(28.1%对 7.9%,p=8.629e-09)。在 26 个候选基因中,5 个基因的 PDVs 患病率在患者和对照组之间存在统计学差异(235 名患者中有 33 名,241 名对照中有 1 名,p=4.533e-10),包括(p=0.0033)、(p=0.0190)、(p=0.0140)、(p=0.0140)和(p=0.0287)。此外,在 POAG 队列中发现了两个携带无义突变 p.Ter494Glu 的姐妹,对该家族的进一步分析强烈表明 p.Ter494Glu 是 POAG 的一种潜在致病突变。在携带 PDVs 的患者和不携带 PDVs 的患者之间发现了诊断时年龄的统计学差异,这表明鉴定的一些 PDVs 可能在促进 POAG 疾病的早期发病中起作用。
结论
结果表明,POAG 风险位点的一些关联可归因于罕见的编码变异,这些变异可能具有功能效应,从而改变 POAG 的风险。
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