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老年人表观遗传年龄加速与认知能力随时间的变化

Epigenetic age acceleration and cognitive performance over time in older adults.

作者信息

Phyo Aung Zaw Zaw, Wu Zimu, Espinoza Sara E, Murray Anne M, Fransquet Peter D, Wrigglesworth Jo, Woods Robyn L, Ryan Joanne

机构信息

Biological Neuropsychiatry & Dementia Unit School of Public Health and Preventive Medicine Monash University Melbourne Victoria Australia.

Department of Medicine Center for Translational Geroscience Cedars-Sinai Medical Center Los Angeles California USA.

出版信息

Alzheimers Dement (Amst). 2024 Sep 14;16(3):e70010. doi: 10.1002/dad2.70010. eCollection 2024 Jul-Sep.

Abstract

INTRODUCTION

This study investigated whether epigenetic age acceleration (AA) is associated with the change in cognitive function and the risk of incident dementia over 9 years, separately in males and females.

METHODS

Six epigenetic AA measures, including GrimAge, were estimated in baseline blood samples from 560 Australians aged ≥70 years (50.7% female). Cognitive assessments included global function, episodic memory, executive function, and psychomotor speed. Composite cognitive scores were also generated. Dementia (Diagnostic and Statistical Manual for Mental Disorders - IV [DSM-IV] criteria) was adjudicated by international experts.

RESULTS

Associations between epigenetic AA and cognitive performance over-time varied by sex. In females only, GrimAA/Grim2AA was associated with worse delayed recall, composite cognition, and composite memory (adjusted-beta ranged from -0.1372 to -0.2034). In males only, GrimAA/Grim2AA was associated with slower processing speed (adjusted-beta, -0.3049) and increased dementia risk (adjusted hazard ratios [HRs], 1.78 and 2.00, respectively).

DISCUSSION

Epigenetic AA is associated with cognitive deterioration in later life but with evidence of sex-specific associations.

HIGHLIGHTS

Epigenetic age acceleration was associated with cognitive deterioration over time.However, these associations differed by sex.In females, accelerated GrimAge appeared to be a better marker of decline in memory.In males, accelerated GrimAge was associated with slower processing speed over time.Association between accelerated GrimAge and dementia risk was found only in males.

摘要

引言

本研究调查了表观遗传年龄加速(AA)是否与9年间认知功能的变化以及新发痴呆症的风险相关,分别在男性和女性中进行了研究。

方法

在来自560名年龄≥70岁的澳大利亚人(50.7%为女性)的基线血液样本中,估计了六种表观遗传AA指标,包括GrimAge。认知评估包括整体功能、情景记忆、执行功能和精神运动速度。还生成了综合认知分数。痴呆症(根据《精神疾病诊断与统计手册》第四版[DSM-IV]标准)由国际专家判定。

结果

表观遗传AA与随时间变化的认知表现之间的关联因性别而异。仅在女性中,GrimAA/Grim2AA与较差的延迟回忆、综合认知和综合记忆相关(调整后的β范围为-0.1372至-0.2034)。仅在男性中,GrimAA/Grim2AA与较慢的处理速度相关(调整后的β为-0.3049)以及痴呆症风险增加(调整后的风险比[HRs]分别为1.78和2.00)。

讨论

表观遗传AA与晚年认知功能衰退相关,但有性别特异性关联的证据。

要点

表观遗传年龄加速与随时间的认知衰退相关。然而,这些关联因性别而异。在女性中,加速的GrimAge似乎是记忆衰退的更好指标。在男性中,加速的GrimAge与随时间推移较慢的处理速度相关。仅在男性中发现加速的GrimAge与痴呆症风险之间的关联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f81c/11399883/4b713c6fc7d9/DAD2-16-e70010-g001.jpg

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