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与中风相关的脑小血管病中的动脉、静脉及脑脊液流动与搏动性:一项纵向分析

Arterial, Venous, and Cerebrospinal Fluid Flow and Pulsatility in Stroke-Related Cerebral Small Vessel Disease: A Longitudinal Analysis.

作者信息

Morgan Alasdair G, Thrippleton Michael J, Stringer Michael S, Chappell Francesca M, Valdés-Hernández Maria C, Wiseman Stewart, Ballerini Lucia, Brown Rosalind, Cheng Yajun, Liu Xiaodi, Zhang Junfang, Sakka Eleni, Jamie Garcia Daniela, Sleight Emilie, Manning Cameron, Coello Roberto D, Job Dominic, Jochems Angela, Arteaga Reyes Carmen, Clancy Una, Marshall Ian, Doubal Fergus N, Wardlaw Joanna M

机构信息

Department of Neuroimaging Sciences, Centre for Clinical Brain Sciences, The University of Edinburgh, United Kingdom (A.G.M., M.J.T., M.S.S., F.M.C., M.C.V.-H., S.W., R.B., E. Sakka, D.J.G., E. Sleight, C.M., R.D.C., D.J., A.J., C.A.R., U.C., I.M., F.N.D., J.M.W.).

UK Dementia Research Institute at The University of Edinburgh, Edinburgh Medical School, United Kingdom (A.G.M., M.J.T., M.S.S., F.M.C., M.C.V.-H., S.W., R.B., E. Sakka, D.J.G., E. Sleight, C.M., R.D.C., D.J., A.J., C.A.R., U.C., I.M., F.N.D., J.M.W.).

出版信息

Stroke. 2025 Sep;56(9):2450-2463. doi: 10.1161/STROKEAHA.124.049103. Epub 2025 Jun 18.

Abstract

BACKGROUND

Cerebral small vessel disease (SVD) causes up to 45% of dementias and 25% of ischemic strokes, but the understanding of vascular pathophysiology is limited. We aimed to investigate the contribution of pulsatility of intracranial arteries, veins, and cerebrospinal fluid (CSF) and cerebral blood flow to long-term imaging and clinical outcomes in SVD.

METHODS

We prospectively recruited participants in Edinburgh/Lothian, Scotland, with lacunar or nonlacunar ischemic stroke (modified Rankin Scale score ≤2, as controls) and assessed medical and brain magnetic resonance imaging characteristics at baseline and 1 year (2018-2022). We used phase-contrast magnetic resonance imaging to measure flow and pulsatility in major cerebral vessels and CSF to investigate independent associations with baseline white matter hyperintensity (WMH) and perivascular space (PVS) volumes and their progression, as well as with recurrent stroke, functional, and cognitive outcomes at 1 year. We applied linear, logistic, and ordinal regression models in our analysis.

RESULTS

We recruited 210 participants; 205 (66.8% male; aged 66.4±11.1 years) had useable data. In covariate-adjusted analyses, higher baseline arterial pulsatility was associated with larger volumes of baseline WMH (B=0.26 [95% CI, 0.08-0.44]; =0.01) and basal ganglia PVS (B=0.12 [95% CI, 0.04-0.20]; <0.01) but not with their change at 1 year (WMH: B=0.01 [95% CI, -0.05 to 0.06]; =0.78; basal ganglia PVS: B=0.02 [95% CI, -0.04 to -0.07]; =0.62) or cognition, dependency, or recurrent stroke at 1 year. Neither cerebral blood flow nor CSF pulsatility was related to baseline SVD severity, WMH/PVS progression, or clinical outcomes at 1 year.

CONCLUSIONS

Associations between vascular/CSF pulsatility, cerebral blood flow, WMH/PVS, and clinical SVD features are complex. The lack of association between intracranial arterial, venous, or CSF pulsatility, cerebral blood flow, and WMH or PVS longitudinal change in this large, covariate-adjusted analysis questions the presumption that high intracranial vascular pulsatility causes SVD and its progression, consistent with other recent longitudinal studies. Intracranial pulsatility may differ from systemic vascular measures in their cause-pathogenic role(s) in SVD and should be considered separately.

摘要

背景

脑小血管病(SVD)导致高达45%的痴呆症和25%的缺血性中风,但对其血管病理生理学的了解有限。我们旨在研究颅内动脉、静脉和脑脊液(CSF)的搏动性以及脑血流量对SVD长期影像学和临床结局的影响。

方法

我们在苏格兰爱丁堡/洛锡安区前瞻性招募了腔隙性或非腔隙性缺血性中风患者(改良Rankin量表评分≤2,作为对照),并在基线和1年(2018 - 2022年)评估其医学和脑磁共振成像特征。我们使用相位对比磁共振成像测量大脑主要血管和脑脊液中的血流和搏动性,以研究其与基线白质高信号(WMH)和血管周围间隙(PVS)体积及其进展的独立关联,以及与1年时复发性中风、功能和认知结局的关联。我们在分析中应用了线性、逻辑和有序回归模型。

结果

我们招募了210名参与者;205名(66.8%为男性;年龄66.4±11.1岁)有可用数据。在协变量调整分析中,较高的基线动脉搏动性与更大的基线WMH体积(B = 0.26 [95% CI,0.08 - 0.44];P = 0.01)和基底节PVS体积(B = 0.12 [95% CI,0.04 - 0.20];P < 0.01)相关,但与1年时它们的变化无关(WMH:B = 0.01 [95% CI, - 0.05至0.06];P = 0.78;基底节PVS:B = 0.02 [95% CI, - 0.04至 - 0.07];P = 0.62),也与1年时的认知、依赖或复发性中风无关。脑血流量和脑脊液搏动性均与基线SVD严重程度、WMH/PVS进展或1年时的临床结局无关。

结论

血管/脑脊液搏动性、脑血流量、WMH/PVS与临床SVD特征之间的关联很复杂。在这项大型协变量调整分析中,颅内动脉、静脉或脑脊液搏动性、脑血流量与WMH或PVS纵向变化之间缺乏关联,这对高颅内血管搏动性导致SVD及其进展的假设提出了质疑,这与其他近期纵向研究一致。颅内搏动性在SVD的病因 - 致病作用方面可能与全身血管测量不同,应分别考虑。

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