Association of Mitochondrial DNA Copy Number With Brain MRI Markers and Cognitive Function

痴呆 孟德尔随机化 队列 认知功能衰退 混淆 线粒体DNA 认知 医学 内表型 阿尔茨海默病 内科学 生物信息学 遗传学 生物 疾病 精神科 基因型 遗传变异 基因
作者
Yuankai Zhang,Xue Li,Kerri L. Wiggins,Nuzulul Kurniansyah,Xiuqing Guo,Amanda Rodrigue,Wei Zhao,Lisa R. Yanek,Scott M. Ratliff,Achilleas Pitsillides,Juan Sebastian Aguirre Patiño,Tamar Sofer,Dan E. Arking,Thomas R. Austin,Alexa S. Beiser,John Blangero,Eric Boerwinkle,Jan Bressler,Joanne E. Curran,Lifang Hou,Timothy M. Hughes,Sharon L. R. Kardia,Lenore J. Launer,Daniel Levy,Thomas H. Mosley,Ilya M. Nasrallah,Stephen S. Rich,Jerome I. Rotter,Sudha Seshadri,Wassim Tarraf,Kevin A. González,Ramachandran S. Vasan,Kristine Yaffe,Paul Nyquist,Bruce M. Psaty,Charles DeCarli,Jennifer A. Smith,David C. Glahn,Héctor M. González,Joshua C. Bis,Myriam Fornage,Susan R. Heckbert,Annette L. Fitzpatrick,Chunyu Liu,Claudia L. Satizábal,Núria Aguilera,Seth A. Ament,Farah Ammous,Donna K. Arnett,Diane M. Becker,Joshua C. Bis,Elizabeth Blue,Eric Boerwinkle,Camille Breaux,Jan Bressler,Dima Chaar,MHI,Danielle Clarkson-Townsend,Benjamin Cooper,Josef Coresh,Adolfo Correa,Anita L. DeStefano,Jingzhong Ding,David W. Fardo,Annette L. Fitzpatrick,Myriam Fornage,Jennifer French,David C. Glahn,Héctor M. González,Einat Granot‐Hershkovitz,Patrick J. Hanly,Kathleen M. Hayden,Susan R. Heckbert,Scott Heemann,Steve Horvath,Karin F. Hoth,Timothy M. Hughes,Sidd Jaiswal,Xueqiu Jian,Yuriko Katsumata,Minjung Kho,Charles Kooperberg,Lenore J. Launer,Honghuang Lin,Elizabeth Litkowski,W.T. Longstreth,Alexandra Martin,Richard Mayeux,Julie Mikulla,Amy Miller,Biswapriya B. Misra,Thomas H. Mosley,Paul Nyquist,Jeff O’Connell,Michael Olivier,Gina M. Peloso,James A. Perry,Bruce M. Psaty,Shaun Purcell,Laura M. Raffield,Yugandi Ranaweera,Alex P. Reiner,Jerome I. Rotter,Cécile Duplàa,Chloé Sarnowski,Claudia L. Satizabal,Gerard Schellenberg,Bonnie L Schoenbein,Sudha Seshadri,Lincoln M. P. Shade,Meghan I. Short,Jeannette Simino,Jennifer A. Smith,Moyra Smith,Sylvia Smoller,Beverly M. Snively,Rachel Soemedi,Sophie Sokolow,Daune Thorington,Timothy A. Thornton,Lisa R. Yanek,Qiong Yang,Miao Yu,Habil Zare,Wei Zhao,Gonçalo R. Abecasis,Avinash Abhyankar,Micheala A. Aldred,Dan E. Arking,Allison Ashley-Koch,Abraham Aviv,Kathleen Barnes,Emily Barron‐Casella,Stephanie L. Battle,Thomas W. Blackwell,Deepika Burkardt,Christina A. Castellani,Suzy Comhair,Benjamin Cooper,Adolfo Correa,Pernell W. Crockett,Mariza de Andrade,Dawn L. DeMeo,M Depaoli,Jun Ding,Christine Dobski,Serpil C. Erzurum,Samar Farha,Jessica L. Fetterman,Caitlin Floyd,Mao Fu,Anthea C. Gist,Einat Granot‐Hershkovitz,C. Charles Gu,Scott Heemann,Ryan D. Hernandez,Yun Soo Hong,Yi‐Hsiang Hsu,Anne E. Justice,Leslie A. Lange,Dan Levy,Honghuang Lin,Chunyu Liu,Ryan J. Longchamps,Jian-Fang Ma,JoAnn Manson,Tiffanie Markus,Merry‐Lynn McDonald,Stephen T. McGarvey,Julie Mikulla,Courtney G. Montgomery,Rajeeva Musunuri,Jeff O’Connell,Richard Oppong,Nathan Pankratz,Yong Qian,Jerome I. Rotter,Scott M. Ratliff,Albert V. Smith,Tamar Sofer,Elizabeth A. Streeten,Weihong Tang,Kent D. Taylor,Marilyn J. Telen,Shelby Thompson,Daune Thorington,Hemant K. Tiwari,Ann Walsh,Emily S. Wan,Jingwen Chen,Heming Wang,Penglong Wang,B. S. Weir,L. Keoki Williams,James G. Wilson,Shujie Xiao,Weiling Xu,Yang Yi,Wei Zhao
出处
期刊:Neurology [Lippincott Williams & Wilkins]
卷期号:100 (18) 被引量:4
标识
DOI:10.1212/wnl.0000000000207157
摘要

Previous studies suggest that lower mitochondrial DNA (mtDNA) copy number (CN) is associated with neurodegenerative diseases. However, whether mtDNA CN in whole blood is related to endophenotypes of Alzheimer disease (AD) and AD-related dementia (AD/ADRD) needs further investigation. We assessed the association of mtDNA CN with cognitive function and MRI measures in community-based samples of middle-aged to older adults.We included dementia-free participants from 9 diverse community-based cohorts with whole-genome sequencing in the Trans-Omics for Precision Medicine (TOPMed) program. Circulating mtDNA CN was estimated as twice the ratio of the average coverage of mtDNA to nuclear DNA. Brain MRI markers included total brain, hippocampal, and white matter hyperintensity volumes. General cognitive function was derived from distinct cognitive domains. We performed cohort-specific association analyses of mtDNA CN with AD/ADRD endophenotypes assessed within ±5 years (i.e., cross-sectional analyses) or 5-20 years after blood draw (i.e., prospective analyses) adjusting for potential confounders. We further explored associations stratified by sex and age (<60 vs ≥60 years). Fixed-effects or sample size-weighted meta-analyses were performed to combine results. Finally, we performed mendelian randomization (MR) analyses to assess causality.We included up to 19,152 participants (mean age 59 years, 57% women). Higher mtDNA CN was cross-sectionally associated with better general cognitive function (β = 0.04; 95% CI 0.02-0.06) independent of age, sex, batch effects, race/ethnicity, time between blood draw and cognitive evaluation, cohort-specific variables, and education. Additional adjustment for blood cell counts or cardiometabolic traits led to slightly attenuated results. We observed similar significant associations with cognition in prospective analyses, although of reduced magnitude. We found no significant associations between mtDNA CN and brain MRI measures in meta-analyses. MR analyses did not reveal a causal relation between mtDNA CN in blood and cognition.Higher mtDNA CN in blood is associated with better current and future general cognitive function in large and diverse communities across the United States. Although MR analyses did not support a causal role, additional research is needed to assess causality. Circulating mtDNA CN could serve nevertheless as a biomarker of current and future cognitive function in the community.
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