Higher Hospital Frailty Risk Score Is Associated With Increased Risk of Stroke: Observational and Genetic Analyses

医学 冲程(发动机) 观察研究 孟德尔随机化 知情同意 老年学 内科学 替代医学 遗传变异 病理 生物化学 机械工程 基因 工程类 基因型 化学
作者
Daniela Renedo,Julián Acosta,Andrew B. Koo,Cyprien Rivier,Nanthiya Sujijantarat,Adam de Havenon,Richa Sharma,Thomas M. Gill,Kevin N Sheth,Guido J Falcone,Charles Matouk
出处
期刊:Stroke [Ovid Technologies (Wolters Kluwer)]
卷期号:54 (6): 1538-1547
标识
DOI:10.1161/strokeaha.122.041891
摘要

Background: Frailty is a prevalent state associated with several aging-related traits and conditions. The relationship between frailty and stroke remains understudied. Here we aim to investigate whether the hospital frailty risk score (HFRS) is associated with the risk of stroke and determine whether a significant association between genetically determined frailty and stroke exists. Design: Observational study using data from All of Us research program and Mendelian Randomization analyses. Methods: Participants from All of Us with available electronic health records were selected for analysis. All of Us began national enrollment in 2018 and is expected to continue for at least 10 years. All of Us is recruiting members of groups that have traditionally been underrepresented in research. All participants provided informed consent at the time of enrollment, and the date of consent was recorded for each participant. Incident stroke was defined as stroke event happening on or after the date of consent to the All of Us study HFRS was measured with a 3-year look-back period before the date of consent for stroke risk. The HFRS was stratified into 4 categories: no-frailty (HFRS=0), low (HFRS ≥1 and <5), intermediate (≥5 and <15), and high (HFRS ≥15). Last, we implemented Mendelian Randomization analyses to evaluate whether genetically determined frailty is associated with stroke risk. Results: Two hundred fifty-three thousand two hundred twenty-six participants were at risk of stroke. In multivariable analyses, frailty status was significantly associated with risk of any (ischemic or hemorrhagic) stroke following a dose-response way: not-frail versus low HFRS (HR, 4.9 [CI, 3.5–6.8]; P <0.001), not-frail versus intermediate HFRS (HR, 11.4 [CI, 8.3–15.7]; P <0.001) and not-frail versus high HFRS (HR, 42.8 [CI, 31.2–58.6]; P <0.001). We found similar associations when evaluating ischemic and hemorrhagic stroke separately ( P value for all comparisons <0.05). Mendelian Randomization confirmed this association by indicating that genetically determined frailty was independently associated with risk of any stroke (OR, 1.45 [95% CI, 1.15–1.84]; P =0.002). Conclusions: Frailty, based on the HFRS was associated with higher risk of any stroke. Mendelian Randomization analyses confirmed this association providing evidence to support a causal relationship.
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