Genetic Variation and Stroke Recovery: The STRONG Study

医学 冲程(发动机) 邦费罗尼校正 改良兰金量表 内科学 物理疗法 机械工程 工程类 统计 缺血性中风 数学 缺血
作者
Steven C. Cramer,Livia Parodi,Zahra Moslemi,Robynne Braun,Chad Aldridge,Babak Shahbaba,Jonathan Rosand,E. Alison Holman,Shreyansh Shah,Christoph J. Griessenauer,Nirav Patel,Christopher D. Anderson,Jonathan J. Henry,Christina Kourkoulis,David J. Lin,Natalie O. Zaba,Joey Gee,Johnson Moon,Julie Schwertfeger,Arun Jayaraman,Robert Lee,Maarten G. Lansberg,Stephanie Kemp,Emily Huang,Elijah Bingham,Leonel Lugo,Da Eun Eun,Jeremy Payne,Carolynn Patten,Kwan Ng,Madelyn Cao,Ashley Jubb,Breann McGee,Ryan Shahbaba,Kunal Agrawal,Brett Kissela,Stacey L. DeJong,John A. Cole,Brian Silver,Christina Manxhari,Brett Cucchiara,Ania Busza,Jennifer Paige Hepple,Sook‐Lei Liew,Susan Alderman,Jennifer E. S. Beauchamp,Nitha Joseph Mathew,Heather Hayes,Jennifer J. Majersik,Bradford B. Worrall,David Tirschwell,Cheryl Bushnell,Nada El Husseini,Jin‐Moo Lee,Guido J. Falcone
出处
期刊:Stroke [Lippincott Williams & Wilkins]
卷期号:55 (8): 2094-2102 被引量:2
标识
DOI:10.1161/strokeaha.124.047643
摘要

BACKGROUND: Genetic association studies can reveal biology and treatment targets but have received limited attention for stroke recovery. STRONG (Stroke, Stress, Rehabilitation, and Genetics) was a prospective, longitudinal (1-year), genetic study in adults with stroke at 28 US stroke centers. The primary aim was to examine the association that candidate genetic variants have with (1) motor/functional outcomes and (2) stress-related outcomes. METHODS: For motor/functional end points, 3 candidate gene variants (ApoE ε4, BDNF [brain-derived neurotrophic factor], and a dopamine polygenic score) were analyzed for associations with change in grip strength (3 months-baseline), function (3-month Stroke Impact Scale-Activities of Daily Living), mood (3-month Patient Health Questionnaire-8), and cognition (12-month telephone-Montreal Cognitive Assessment). For stress-related outcomes, 7 variants (serotonin transporter gene–linked promoter region, ACE [angiotensin-converting enzyme], oxytocin receptor, FKBP5 [FKBP prolyl isomerase 5], FAAH [fatty acid amide hydrolase], BDNF, and COMT [catechol-O-methyltransferase]) were assessed for associations with posttraumatic stress disorder ([PTSD]; PTSD Primary Care Scale) and depression (Patient Health Questionnaire-8) at 6 and 12 months; stress-related genes were examined as a function of poststroke stress level. Statistical models (linear, negative binomial, or Poisson regression) were based on response variable distribution; all included stroke severity, age, sex, and ancestry as covariates. Stroke subtype was explored secondarily. Data were Holm-Bonferroni corrected. A secondary replication analysis tested whether the rs1842681 polymorphism (identified in the GISCOME study [Genetics of Ischaemic Stroke Functional Outcome]) was related to 3-month modified Rankin Scale score in STRONG. RESULTS: The 763 enrollees were 63.1±14.9 (mean±SD) years of age, with a median initial National Institutes of Health Stroke Scale score of 4 (interquartile range, 2–9); outcome data were available in n=515 at 3 months, n=500 at 6 months, and n=489 at 12 months. At 1 year poststroke, the rs6265 (BDNF) variant was associated with poorer cognition (0.9-point lower telephone-Montreal Cognitive Assessment score, P =1×10 −5 ). For stress-related outcomes, rs4291 (ACE) and rs324420 (FAAH) were risk factors linking increased poststroke stress with higher 1-year depression and PTSD symptoms ( P <0.05), while rs4680 (COMT) linked poststroke stress with lower 1-year depression and PTSD. Findings were unchanged when considering stroke subtype. STRONG replicated GISCOME: rs1842681 was associated with lower 3-month modified Rankin Scale score ( P =3.2×10 −5 ). CONCLUSIONS: This study identified genetic associations with cognitive function, depression, and PTSD 1 year poststroke. Genetic susceptibility to PTSD and depressive symptoms varied according to the amount of poststroke stress, underscoring the critical role of lived experiences in recovery. Together, the results suggest that genetic association studies provide insights into the biology of stroke recovery in humans.

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