Genome-Wide Genetic Analysis of Dropout in a Controlled Exercise Intervention in Sedentary Adults With Overweight or Obesity and Cardiometabolic Disease.

IF 3.6 2区 心理学 Q1 PSYCHOLOGY, MULTIDISCIPLINARY Annals of Behavioral Medicine Pub Date : 2024-04-11 DOI:10.1093/abm/kaae011
Rong Jiang, Katherine A Collins, Kim M Huffman, Elizabeth R Hauser, Monica J Hubal, Johanna L Johnson, Redford B Williams, Ilene C Siegler, William E Kraus
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Abstract

Background: Despite the benefits of exercise, many individuals are unable or unwilling to adopt an exercise intervention.

Purpose: The purpose of this analysis was to identify putative genetic variants associated with dropout from exercise training interventions among individuals in the STRRIDE trials.

Methods: We used a genome-wide association study approach to identify genetic variants in 603 participants initiating a supervised exercise intervention. Exercise intervention dropout occurred when a subject withdrew from further participation in the study or was otherwise lost to follow-up.

Results: Exercise intervention dropout was associated with a cluster of single-nucleotide polymorphisms with the top candidate being rs722069 (T/C, risk allele = C) (unadjusted p = 2.2 × 10-7, odds ratio = 2.23) contained within a linkage disequilibrium block on chromosome 16. In Genotype-Tissue Expression, rs722069 is an expression quantitative trait locus of the EARS2, COG7, and DCTN5 genes in skeletal muscle tissue. In subsets of the STRRIDE genetic cohort with available muscle gene expression (n = 37) and metabolic data (n = 82), at baseline the C allele was associated with lesser muscle expression of EARS2 (p < .002) and COG7 (p = .074) as well as lesser muscle concentrations of C2- and C3-acylcarnitines (p = .026).

Conclusions: Our observations imply that exercise intervention dropout is genetically moderated through alterations in gene expression and metabolic pathways in skeletal muscle. Individual genetic traits may allow the development of a biomarker-based approach for identifying individuals who may benefit from more intensive counseling and other interventions to optimize exercise intervention adoption.

Clinical trial information: STRRIDE I = NCT00200993; STRRIDE AT/RT = NCT00275145; STRRIDE-PD = NCT00962962.

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对患有超重或肥胖症及心脏代谢疾病的久坐成人退出受控运动干预的全基因组遗传分析。
背景:目的:本分析的目的是确定与 STRRIDE 试验中个人退出运动训练干预相关的假定遗传变异:我们采用全基因组关联研究的方法,在 603 名开始接受监督锻炼干预的参与者中识别基因变异。当受试者不再继续参与研究或因其他原因失去随访机会时,就会退出运动干预:结果:运动干预退出与一组单核苷酸多态性有关,其中最大的候选基因是rs722069(T/C,风险等位基因=C)(未调整p=2.2×10-7,几率比=2.23),该基因包含在16号染色体上的一个连锁不平衡区块中。在基因型-组织表达中,rs722069 是骨骼肌组织中 EARS2、COG7 和 DCTN5 基因的表达定量性状位点。在具有肌肉基因表达(n = 37)和代谢数据(n = 82)的 STRRIDE 遗传队列子集中,在基线时,C 等位基因与较低的 EARS2(p < .002)和 COG7(p = .074)肌肉表达以及较低的 C2-和 C3-酰肉碱肌肉浓度(p = .026)相关:我们的观察结果表明,通过改变骨骼肌中的基因表达和代谢途径,运动干预辍学会受到遗传因素的调节。个体遗传特征可能有助于开发一种基于生物标志物的方法,用于识别可能从更深入的咨询和其他干预措施中获益的个体,以优化运动干预措施的采用:strride i = NCT00200993; strride at/rt = NCT00275145; strride-pd = NCT00962962.
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来源期刊
Annals of Behavioral Medicine
Annals of Behavioral Medicine PSYCHOLOGY, MULTIDISCIPLINARY-
CiteScore
7.00
自引率
5.30%
发文量
65
期刊介绍: Annals of Behavioral Medicine aims to foster the exchange of knowledge derived from the disciplines involved in the field of behavioral medicine, and the integration of biological, psychosocial, and behavioral factors and principles as they relate to such areas as health promotion, disease prevention, risk factor modification, disease progression, adjustment and adaptation to physical disorders, and rehabilitation. To achieve these goals, much of the journal is devoted to the publication of original empirical articles including reports of randomized controlled trials, observational studies, or other basic and clinical investigations. Integrative reviews of the evidence for the application of behavioral interventions in health care will also be provided. .
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