Strategic infarct locations for post-stroke cognitive impairment: a pooled analysis of individual patient data from 12 acute ischaemic stroke cohorts

医学 冲程(发动机) 神经心理学 体素 认知 内科学 神经心理评估 队列 心脏病学 物理疗法 物理医学与康复 放射科 精神科 机械工程 工程类
作者
Nick A. Weaver,Hugo J. Kuijf,Hugo P. Aben,Jill Abrigo,Hee Joon Bae,Mélanie Barbay,Jonathan G. Best,Régis Bordet,Francesca M Chappell,Christopher Chen,Thibaut Dondaine,Ruben S. van der Giessen,Olivier Godefroy,Bibek Gyanwali,Olivia Hamilton,Saima Hilal,Irene M.C. Huenges Wajer,Yeonwook Kang,L. Jaap Kappelle,Beom Joon Kim,Sebastian Köhler,Paul L.M. de Kort,Peter J. Koudstaal,Grégory Kuchcinski,Bonnie Yin Ka Lam,Byung Chul Lee,Keon Joo Lee,Jae‐Sung Lim,Renaud Lopes,Stephen D. Makin,Anne Marie Mendyk,Vincent Mok,Mi Sun Oh,Robert J. van Oostenbrugge,Martine Roussel,Lin Shi,Julie Staals,Maria del C. Valdés-Hernández,Narayanaswamy Venketasubramanian,Frans R.J. Verhey,Joanna M. Wardlaw,David J. Werring,Xiaoyan Xu,Kyung Ho Yu,M.J.E. van Zandvoort,Lei Zhao,J. Matthijs Biesbroek,Geert Jan Biessels
出处
期刊:Lancet Neurology [Elsevier]
卷期号:20 (6): 448-459 被引量:129
标识
DOI:10.1016/s1474-4422(21)00060-0
摘要

Background Post-stroke cognitive impairment (PSCI) occurs in approximately half of people in the first year after stroke. Infarct location is a potential determinant of PSCI, but a comprehensive map of strategic infarct locations predictive of PSCI is unavailable. We aimed to identify infarct locations most strongly predictive of PSCI after acute ischaemic stroke and use this information to develop a prediction model. Methods In this large-scale multicohort lesion-symptom mapping study, we pooled and harmonised individual patient data from 12 cohorts through the Meta-analyses on Strategic Lesion Locations for Vascular Cognitive Impairment using Lesion-Symptom Mapping (Meta VCI Map) consortium. The identified cohorts (as of Jan 1, 2019) comprised patients with acute symptomatic infarcts on CT or MRI (with available infarct segmentations) and a cognitive assessment up to 15 months after acute ischaemic stroke onset. PSCI was defined as performance lower than the fifth percentile of local normative data, on at least one cognitive domain on a multidomain neuropsychological assessment or on the Montreal Cognitive Assessment. Voxel-based lesion-symptom mapping (VLSM) was used to calculate voxel-wise odds ratios (ORs) for PSCI that were mapped onto a three-dimensional brain template to visualise PSCI risk per location. For the prediction model of PSCI risk, a location impact score on a 5-point scale was derived from the VLSM results on the basis of the mean voxel-wise coefficient (ln[OR]) within each patient's infarct. We did combined internal–external validation by leave-one-cohort-out cross-validation for all 12 cohorts using logistic regression. Predictive performance of a univariable model with only the location impact score was compared with a multivariable model with addition of other clinical PSCI predictors (age, sex, education, time interval between stroke onset and cognitive assessment, history of stroke, and total infarct volume). Testing of visual ratings was done by three clinicians, and accuracy, inter-rater reliability, and intra-rater reliability were assessed with Cohen's weighted kappa. Findings In our sample of 2950 patients (mean age 66·8 years [SD 11·6]; 1157 [39·2%] women), 1286 (43·6%) had PSCI. We achieved high lesion coverage of the brain in our analyses (86·9%). Infarcts in the left frontotemporal lobes, left thalamus, and right parietal lobe were strongly associated with PSCI (after false discovery rate correction, q<0·01; voxel-wise ORs >20). On cross-validation, the location impact score showed good correspondence, based on visual assessment of goodness of fit, between predicted and observed risk of PSCI across cohorts after adjusting for cohort-specific PSCI occurrence. Cross-validations showed that the location impact score by itself had similar performance to the combined model with other PSCI predictors, while allowing for easy visual assessment. Therefore the univariable model with only the location impact score was selected as the final model. Correspondence between visual ratings and actual location impact score (Cohen's weighted kappa: range 0·88–0·92), inter-rater agreement (0·85–0·87), and intra-rater agreement (for a single rater, 0·95) were all high. Interpretation To the best of our knowledge, this study provides the first comprehensive map of strategic infarct locations associated with risk of PSCI. A location impact score was derived from this map that robustly predicted PSCI across cohorts. Furthermore, we developed a quick and reliable visual rating scale that might in the future be applied by clinicians to identify individual patients at risk of PSCI. Funding The Netherlands Organisation for Health Research and Development.
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