全基因组关联和关联分析发现 DLG 相关蛋白-1 是肌肉力量的一个新的位置和生物学候选基因:长寿家族研究

Adam J Santanasto, Sandeep Acharya, Mary K Wojczynski, Ryan K Cvejkus, Shiow Lin, Michael R Brent, Jason A Anema, Lihua Wang, Bharat Thyagarajan, Kaare Christensen, E Warwick Daw, Joseph M Zmuda
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In these 6 families, using whole genome sequencing data, we performed association analyses between the 7 312 single nucleotide (SNVs) and insertion deletion (INDELs) variants in the linkage region and grip strength. Models were adjusted for age, age2, sex, height, field center, and population substructure.</p><p><strong>Results: </strong>We found significant associations between genetic variants (8 SNVs and 4 INDELs, p < 5 × 10-5) in the Disks Large-associated Protein 1 (DLGAP1) gene and grip strength. Haplotypes constructed using these variants explained up to 98.1% of the LOD score. 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引用次数: 0

摘要

背景:握力是整体健康的有力指标,具有中度遗传性,可预测老年人的寿命:握力是衡量总体健康状况的可靠指标,具有中度遗传性,可预测老年人的寿命:通过全基因组关联分析,我们在来自 582 个家庭的 3755 名 64 ± 12 岁(年龄范围 30-110 岁;55% 为女性)的个体中发现了染色体 18p 上与握力相关的一个新位点(巨基对区域:3.4 - 4.0)。有 26 个家族贡献了连接峰值(累积几率对数 [LOD] 得分 = 10.94),其中 6 个家族(119 人)占连接信号的大部分(LOD = 6.4)。在这 6 个家族中,我们利用全基因组测序数据,对连接区的 7312 个单核苷酸(SNV)和插入缺失(INDEL)变异与握力进行了关联分析。模型根据年龄、年龄2、性别、身高、田野中心和人群亚结构进行了调整:结果:我们发现基因变异(8 个 SNV 和 4 个 INDEL,pConclusions)与握力之间存在显着关联:DLGAP1基因在神经元突触后密度中起着重要作用;因此,它既是一个新的位置候选基因,也是一个生物学候选基因,可用于旨在揭示肌肉力量遗传决定因素的后续研究。
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Whole Genome Linkage and Association Analyses Identify DLG Associated Protein-1 as a Novel Positional and Biological Candidate Gene for Muscle Strength: The Long Life Family Study.

Background: Grip strength is a robust indicator of overall health, is moderately heritable, and predicts longevity in older adults.

Methods: Using genome-wide linkage analysis, we identified a novel locus on chromosome 18p (mega-basepair region: 3.4-4.0) linked to grip strength in 3 755 individuals from 582 families aged 64 ± 12 years (range 30-110 years; 55% women). There were 26 families that contributed to the linkage peak (cumulative logarithm of the odds [LOD] score = 10.94), with 6 families (119 individuals) accounting for most of the linkage signal (LOD = 6.4). In these 6 families, using whole genome sequencing data, we performed association analyses between the 7 312 single nucleotide (SNVs) and insertion deletion (INDELs) variants in the linkage region and grip strength. Models were adjusted for age, age2, sex, height, field center, and population substructure.

Results: We found significant associations between genetic variants (8 SNVs and 4 INDELs, p < 5 × 10-5) in the Disks Large-associated Protein 1 (DLGAP1) gene and grip strength. Haplotypes constructed using these variants explained up to 98.1% of the LOD score. Finally, RNAseq data showed that these variants were significantly associated with the expression of nearby Myosin Light Chain 12A (MYL12A), Structural Maintenance of Chromosomes Flexible Hinge Domain Containing 1 (SMCHD1), Erythrocyte Membrane Protein Band 4.1 Like 3 (EPB41L3) genes (p < .0004).

Conclusions: The DLGAP1 gene plays an important role in the postsynaptic density of neurons; thus, it is both a novel positional and biological candidate gene for follow-up studies aimed at uncovering genetic determinants of muscle strength.

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