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季节性情感障碍(SAD)风险与昼夜节律时钟基因变异有关。

Risk for Seasonal Affective Disorder (SAD) Linked to Circadian Clock Gene Variants.

作者信息

Dang Thanh, Russel William A, Saad Tazmilur, Dhawka Luvna, Ay Ahmet, Ingram Krista K

机构信息

Department of Computer Science, Colgate University, Hamilton, NY 13346, USA.

Department of Biology, Colgate University, Hamilton, NY 13346, USA.

出版信息

Biology (Basel). 2023 Dec 15;12(12):1532. doi: 10.3390/biology12121532.

Abstract

Molecular pathways affecting mood are associated with circadian clock gene variants and are influenced, in part, by the circadian clock, but the molecular mechanisms underlying this link are poorly understood. We use machine learning and statistical analyses to determine the circadian gene variants and clinical features most highly associated with symptoms of seasonality and seasonal affective disorder (SAD) in a deeply phenotyped population sample. We report sex-specific clock gene effects on seasonality and SAD symptoms; genotypic combinations of CLOCK3111/ZBTB20 and PER2/PER3B were significant genetic risk factors for males, and CRY2/PER3C and CRY2/PER3-VNTR were significant risk factors for females. Anxiety, eveningness, and increasing age were significant clinical risk factors for seasonality and SAD for females. Protective factors for SAD symptoms (in females only) included single gene variants: CRY1-GG and PER3-VNTR-4,5. Clock gene effects were partially or fully mediated by diurnal preference or chronotype, suggesting multiple indirect effects of clock genes on seasonality symptoms. Interestingly, protective effects of CRY1-GG, PER3-VNTR-4,5, and ZBTB20 genotypes on seasonality and depression were not mediated by chronotype, suggesting some clock variants have direct effects on depressive symptoms related to SAD. Our results support previous links between CRY2, PER2, and ZBTB20 genes and identify novel links for CLOCK and PER3 with symptoms of seasonality and SAD. Our findings reinforce the sex-specific nature of circadian clock influences on seasonality and SAD and underscore the multiple pathways by which clock variants affect downstream mood pathways via direct and indirect mechanisms.

摘要

影响情绪的分子途径与昼夜节律时钟基因变异相关,并且部分受昼夜节律时钟影响,但这种联系背后的分子机制仍知之甚少。我们使用机器学习和统计分析来确定在一个深度表型化的人群样本中,与季节性和季节性情感障碍(SAD)症状关联度最高的昼夜节律基因变异和临床特征。我们报告了性别特异性的时钟基因对季节性和SAD症状的影响;CLOCK3111/ZBTB20和PER2/PER3B的基因型组合是男性的显著遗传风险因素,而CRY2/PER3C和CRY2/PER3-VNTR是女性的显著风险因素。焦虑、晚睡倾向和年龄增长是女性季节性和SAD的显著临床风险因素。SAD症状的保护因素(仅针对女性)包括单基因变异:CRY1-GG和PER3-VNTR-4,5。时钟基因的影响部分或完全由昼夜偏好或生物钟类型介导,这表明时钟基因对季节性症状有多种间接影响。有趣的是,CRY1-GG、PER3-VNTR-4,5和ZBTB20基因型对季节性和抑郁的保护作用不是由生物钟类型介导的,这表明一些时钟变异对与SAD相关的抑郁症状有直接影响。我们的结果支持了先前CRY2、PER2和ZBTB20基因之间的联系,并确定了CLOCK和PER3与季节性和SAD症状的新联系。我们的发现强化了昼夜节律时钟对季节性和SAD影响的性别特异性,并强调了时钟变异通过直接和间接机制影响下游情绪途径的多种途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/708c/10741218/7c791c6cca05/biology-12-01532-g001.jpg

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