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利用高碳酸血症和高氧呼吸挑战校准脑血管反应性的时间延迟的新视角。

A novel perspective to calibrate temporal delays in cerebrovascular reactivity using hypercapnic and hyperoxic respiratory challenges.

机构信息

Centre for Neuroscience Studies, Queen's University, Kingston, ON, Canada.

Department of Radiology, University Medical Center Utrecht, Utrecht, The Netherlands.

出版信息

Neuroimage. 2019 Feb 15;187:154-165. doi: 10.1016/j.neuroimage.2017.11.044. Epub 2017 Dec 5.

Abstract

Redistribution of blood flow across different brain regions, arising from the vasoactive nature of hypercapnia, can introduce errors when examining cerebrovascular reactivity (CVR) response delays. In this study, we propose a novel analysis method to characterize hemodynamic delays in the blood oxygen level dependent (BOLD) response to hypercapnia, and hyperoxia, as a way to provide insight into transient differences in vascular reactivity between cortical regions, and across tissue depths. A pseudo-continuous arterial spin labeling sequence was used to acquire BOLD and cerebral blood flow simultaneously in 19 healthy adults (12 F; 20 ± 2 years) during boxcar CO and O gas inhalation paradigms. Despite showing distinct differences in hypercapnia-induced response delay times (P < 0.05; Bonferroni corrected), grey matter regions showed homogenous hemodynamic latencies (P > 0.05) once calibrated for bolus arrival time derived using non-vasoactive hyperoxic gas challenges. Longer hypercapnic temporal delays were observed as the depth of the white matter tissue increased, although no significant differences in response lag were found during hyperoxia across tissue depth, or between grey and white matter. Furthermore, calibration of hypercapnic delays using hyperoxia revealed that deeper white matter layers may be more prone to dynamic redistribution of blood flow, which introduces response lag times ranging between 1 and 3 s in healthy subjects. These findings suggest that the combination of hypercapnic and hyperoxic gas-inhalation MRI can be used to distinguish between differences in CVR that arise as a result of delayed stimulus arrival time (due to the local architecture of the cerebrovasculature), or preferential blood flow distribution. Calibrated response delays to hypercapnia provide important insights into cerebrovascular physiology, and may be used to correct response delays associated with vascular impairment.

摘要

由于高碳酸血症的血管活性特性,不同脑区之间的血流重新分布会在检查脑血管反应性 (CVR) 时引入误差。在这项研究中,我们提出了一种新的分析方法来描述血氧水平依赖 (BOLD) 对高碳酸血症和高氧反应的血流动力学延迟,以深入了解皮质区域之间以及组织深度之间血管反应性的瞬时差异。伪连续动脉自旋标记序列用于在 19 名健康成年人 (12 名女性;20±2 岁) 中同时采集 BOLD 和脑血流,在箱式 CO 和 O 气体吸入范式期间。尽管在高碳酸血症诱导的反应延迟时间上表现出明显的差异 (P<0.05;经 Bonferroni 校正),但一旦使用非血管活性高氧气体挑战得出的 bolus 到达时间对灰质区域进行校准,就会表现出均匀的血液动力学潜伏期 (P>0.05)。随着白质组织深度的增加,观察到更长的高碳酸血症时间延迟,尽管在整个组织深度的高氧期间,或在灰质和白质之间,没有发现反应滞后的显著差异。此外,使用高氧校准高碳酸血症延迟表明,更深的白质层可能更容易受到血流的动态再分布影响,这会在健康受试者中引入 1 到 3 秒的反应滞后时间。这些发现表明,高碳酸血症和高氧气体吸入 MRI 的结合可用于区分由于刺激到达时间延迟 (由于脑血管的局部结构) 或优先血流分布而导致的 CVR 差异。对高碳酸血症的校准反应延迟提供了对脑血管生理学的重要见解,并可用于校正与血管损伤相关的反应延迟。

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