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鉴定出 13 个新的早发性心肌梗死、高血压或慢性肾脏病易感性基因座。

Identification of 13 novel susceptibility loci for early-onset myocardial infarction, hypertension, or chronic kidney disease.

机构信息

Department of Human Functional Genomics, Advanced Science Research Promotion Center, Mie University, Tsu, Mie 514‑8507, Japan.

Department of Cardiovascular Medicine, Gifu Prefectural Tajimi Hospital, Tajimi, Gifu 507‑8522, Japan.

出版信息

Int J Mol Med. 2018 Nov;42(5):2415-2436. doi: 10.3892/ijmm.2018.3852. Epub 2018 Sep 4.

DOI:10.3892/ijmm.2018.3852
PMID:30226566
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6192728/
Abstract

Early‑onset cardiovascular and renal diseases have a strong genetic component. In the present study, exome‑wide association studies (EWASs) were performed to identify genetic variants that confer susceptibility to early‑onset myocardial infarction (MI), hypertension, or chronic kidney disease (CKD) in Japanese individuals. A total of 8,093 individuals aged ≤65 years was enrolled in the study. The EWASs for MI, hypertension, and CKD were performed in 6,926 subjects (1,152 cases, 5,774 controls), 8,080 subjects (3,444 cases, 4,636 controls), and 2,556 subjects (1,051 cases, 1,505 controls), respectively. Genotyping of single nucleotide polymorphisms (SNPs) was performed with Illumina Human Exome‑12 DNA Analysis BeadChip or Infinium Exome‑24 BeadChip arrays. The associations of allele frequencies for 31,245, 31,276, or 31,514 SNPs that passed quality control to MI, hypertension, and CKD, respectively, was examined with Fisher's exact test. Bonferroni's correction for statistical significance of association was applied to compensate for multiple comparisons of genotypes with MI, hypertension, or CKD. The EWASs of allele frequencies revealed that 25, 11, and 11 SNPs were significantly associated with MI (P<1.60x10‑6), hypertension (P<1.60x10‑6), or CKD (P<1.59x10‑6), respectively. Multivariable logistic regression analysis with adjustment for covariates showed that all 25, 11, and 11 SNPs were significantly associated with MI (P<0.0005), hypertension (P<0.0011), or CKD (P<0.0011), respectively. On examination of the results from previous genome‑wide association studies and linkage disequilibrium of the identified SNPs, 11 loci (TMOD4, COL6A3, ADGRL3‑CXCL8‑MARCH1, OR52E4, TCHP‑GIT2, CCDC63, 12q24.1, OAS3, PLCB2‑VPS33B, GOSR2, ZNF77), six loci (MOB3C‑TMOD4, COL6A3, COL6A5, CXCL8‑MARCH1, NFKBIL1‑6p21.3‑NCR3, PLCB2‑VPS33B), and seven loci (MOB3C‑TMOD4, COL6A3, COL6A5, ADGRL3‑CXCL8‑MARCH1, MUC17, PLCB2‑VPS33B, ZNF77) were identified as novel loci significantly associated with MI, hypertension, and CKD, respectively. Furthermore, six genes (TMOD4, COL6A3, CXCL8, MARCH1, PLCB2, VPS33B) were significantly associated with MI, hypertension and CKD; two genes (ADGRL3, ZNF77) with MI and CKD; and two genes (COL6A5, MOB3C) with hypertension and CKD. Therefore, 13 novel loci (MOB3C‑TMOD4, COL6A3, ADGRL3‑CXCL8‑MARCH1, OR52E4, TCHP‑GIT2, CCDC63, 12q24.1, OAS3, PLCB2‑VPS33B, ZNF77, COL6A5, NFKBIL1‑NCR3, MUC17) were identified that confer susceptibility to early‑onset MI, hypertension, or CKD. The determination of genotypes for the SNPs at these loci may provide informative for assessment of the genetic risk for MI, hypertension, or CKD.

摘要

早发性心血管和肾脏疾病具有很强的遗传成分。在本研究中,进行了外显子组全基因组关联研究(EWAS),以鉴定在日本人群中导致早发性心肌梗死(MI)、高血压或慢性肾脏病(CKD)易感性的遗传变异。共纳入 8093 名年龄≤65 岁的个体。在 6926 名受试者(1152 例,5774 名对照)、8080 名受试者(3444 例,4636 名对照)和 2556 名受试者(1051 例,1505 名对照)中进行了 MI、高血压和 CKD 的 EWAS。使用 Illumina Human Exome-12 DNA Analysis BeadChip 或 Infinium Exome-24 BeadChip 阵列进行单核苷酸多态性(SNP)的基因分型。Fisher 精确检验用于检查通过质量控制的 31245、31276 或 31514 个 SNP 的等位基因频率与 MI、高血压和 CKD 的关联。Bonferroni 校正用于校正与 MI、高血压或 CKD 的基因型进行多次比较的统计学显著性。等位基因频率的 EWAS 显示,25、11 和 11 个 SNP 分别与 MI(P<1.60x10-6)、高血压(P<1.60x10-6)或 CKD(P<1.59x10-6)显著相关。多变量逻辑回归分析调整了协变量,结果显示所有 25、11 和 11 个 SNP 均与 MI(P<0.0005)、高血压(P<0.0011)或 CKD(P<0.0011)显著相关。对先前全基因组关联研究的结果和鉴定 SNP 的连锁不平衡进行检查,确定了 11 个位点(TMOD4、COL6A3、ADGRL3-CXCL8-MARCH1、OR52E4、TCHP-GIT2、CCDC63、12q24.1、OAS3、PLCB2-VPS33B、GOSR2、ZNF77)、6 个位点(MOB3C-TMOD4、COL6A3、COL6A5、CXCL8-MARCH1、NFKBIL1-6p21.3-NCR3、PLCB2-VPS33B)和 7 个位点(MOB3C-TMOD4、COL6A3、COL6A5、ADGRL3-CXCL8-MARCH1、MUC17、PLCB2-VPS33B、ZNF77)与 MI、高血压和 CKD 显著相关,分别为新的位点。此外,6 个基因(TMOD4、COL6A3、CXCL8、MARCH1、PLCB2、VPS33B)与 MI、高血压和 CKD 显著相关;2 个基因(ADGRL3、ZNF77)与 MI 和 CKD 相关;2 个基因(COL6A5、MOB3C)与高血压和 CKD 相关。因此,鉴定出 13 个新的位点(MOB3C-TMOD4、COL6A3、ADGRL3-CXCL8-MARCH1、OR52E4、TCHP-GIT2、CCDC63、12q24.1、OAS3、PLCB2-VPS33B、ZNF77、COL6A5、NFKBIL1-NCR3、MUC17),这些位点赋予了早发性 MI、高血压或 CKD 的易感性。这些位点的 SNP 基因型的确定可能为 MI、高血压或 CKD 的遗传风险评估提供信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81f8/6192728/28d06b05a801/IJMM-42-05-2415-g01.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81f8/6192728/3a813f626e23/IJMM-42-05-2415-g00.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81f8/6192728/28d06b05a801/IJMM-42-05-2415-g01.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81f8/6192728/3a813f626e23/IJMM-42-05-2415-g00.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81f8/6192728/28d06b05a801/IJMM-42-05-2415-g01.jpg

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