中重度急性外伤性神经损伤中RAP与多模态脑生理动力学的关系:CAHR-TBI多变量分析

IF 3.7 3区 医学 Q2 ENGINEERING, BIOMEDICAL
Abrar Islam, Kevin Y Stein, Donald Griesdale, Mypinder Sekhon, Rahul Raj, Francis Bernard, Clare Gallagher, Eric P Thelin, Francois Mathieu, Andreas Kramer, Marcel Aries, Logan Froese, Frederick A Zeiler
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引用次数: 0

摘要

背景:脑顺应性(或代偿储备)指数RAP是中重度创伤性脑损伤(TBI)治疗中一个重要但未被充分利用的生理指标。虽然RAP有望作为一种连续的床边指标,但其更广泛的大脑生理背景仍有待部分了解。本研究旨在描述RAP受损与大脑生理其他关键组成部分的关系。方法:采用描述性和基于阈值的方法对379例中重度TBI患者的存档数据进行分析,分析了三种RAP状态(受损、完整/过渡和耗尽)。采用聚类层次聚类、主成分分析和基于核的聚类来探索多元协方差结构。然后,使用矢量自回归积分移动平均脉冲响应函数(VARIMA IRF)、相互关系和格兰杰因果关系等高频时间分析来评估RAP与其他生理信号之间的动态耦合。结果:RAP状态受损和耗尽与颅内压升高相关(p = 0.021)。对于AMP, RAP受损与水平升高相关,而RAP耗尽与脉冲幅度降低相关(p = 3.94 × 10-9)。这两种RAP状态也与自我调节受损和灌注减少有关。聚类分析一致将RAP按照其组成信号(ICP和AMP)进行分组,其次是脑氧合参数(脑组织氧合(PbtO2)和区域脑氧饱和度(rSO2))。在自我调节状态受损的情况下,大脑自调节(CA)指数与RAP更接近。时间分析显示,在1分钟分辨率下,RAP对ICP和动脉血压(ABP)表现出相对较强的反应。此外,当比较icp衍生的CA指数和近红外光谱(NIRS)衍生的CA指数时,它们更接近RAP, RAP在高频时间分析中对这些icp衍生的CA指数的变化表现出更大的敏感性。这些趋势在较低的时间分辨率下也保持一致。结论:RAP与其他参数的关系在不同的依从状态下保持一致,但存在有意义的差异。将RAP整合到患者轨迹建模中,并基于不同RAP状态的这些发现开发预测框架,可以绘制出大脑生理学随时间的演变。这种方法可以改善预测和指导个体化干预TBI管理。因此,这些发现支持RAP作为床边监测的有价值指标的潜力,以及它在指导TBI患者轨迹建模和介入研究中的潜在作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Relationship Between RAP and Multi-Modal Cerebral Physiological Dynamics in Moderate/Severe Acute Traumatic Neural Injury: A CAHR-TBI Multivariate Analysis.

Background: The cerebral compliance (or compensatory reserve) index, RAP, is a critical yet underutilized physiological marker in the management of moderate-to-severe traumatic brain injury (TBI). While RAP offers promise as a continuous bedside metric, its broader cerebral physiological context remains partly understood. This study aims to characterize the burden of impaired RAP in relation to other key components of cerebral physiology.

Methods: Archived data from 379 moderate-to-severe TBI patients were analyzed using descriptive and threshold-based methods across three RAP states (impaired, intact/transitional, and exhausted). Agglomerative hierarchical clustering, principal component analysis, and kernel-based clustering were applied to explore multivariate covariance structures. Then, high-frequency temporal analyses, including vector autoregressive integrated moving average impulse response functions (VARIMA IRF), cross-correlation, and Granger causality, were performed to assess dynamic coupling between RAP and other physiological signals.

Results: Impaired and exhausted RAP states were associated with elevated intracranial pressure (p = 0.021). Regarding AMP, impaired RAP was associated with elevated levels, while exhausted RAP was associated with reduced pulse amplitude (p = 3.94 × 10-9). These two RAP states were also associated with compromised autoregulation and diminished perfusion. Clustering analyses consistently grouped RAP with its constituent signals (ICP and AMP), followed by brain oxygenation parameters (brain tissue oxygenation (PbtO2) and regional cerebral oxygen saturation (rSO2)). Cerebral autoregulation (CA) indices clustered more closely with RAP under impaired autoregulatory states. Temporal analyses revealed that RAP exhibited comparatively stronger responses to ICP and arterial blood pressure (ABP) at 1-min resolution. Moreover, when comparing ICP-derived and near-infrared spectroscopy (NIRS)-derived CA indices, they clustered more closely to RAP, and RAP demonstrated greater sensitivity to changes in these ICP-derived CA indices in high-frequency temporal analyses. These trends remained consistent at lower temporal resolutions as well.

Conclusion: RAP relationships with other parameters remain consistent and differ meaningfully across compliance states. Integrating RAP into patient trajectory modelling and developing predictive frameworks based on these findings across different RAP states can map the evolution of cerebral physiology over time. This approach may improve prognostication and guide individualized interventions in TBI management. Therefore, these findings support RAP's potential as a valuable metric for bedside monitoring and its prospective role in guiding patient trajectory modeling and interventional studies in TBI.

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来源期刊
Bioengineering
Bioengineering Chemical Engineering-Bioengineering
CiteScore
4.00
自引率
8.70%
发文量
661
期刊介绍: Aims Bioengineering (ISSN 2306-5354) provides an advanced forum for the science and technology of bioengineering. It publishes original research papers, comprehensive reviews, communications and case reports. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. All aspects of bioengineering are welcomed from theoretical concepts to education and applications. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. There are, in addition, four key features of this Journal: ● We are introducing a new concept in scientific and technical publications “The Translational Case Report in Bioengineering”. It is a descriptive explanatory analysis of a transformative or translational event. Understanding that the goal of bioengineering scholarship is to advance towards a transformative or clinical solution to an identified transformative/clinical need, the translational case report is used to explore causation in order to find underlying principles that may guide other similar transformative/translational undertakings. ● Manuscripts regarding research proposals and research ideas will be particularly welcomed. ● Electronic files and software regarding the full details of the calculation and experimental procedure, if unable to be published in a normal way, can be deposited as supplementary material. ● We also accept manuscripts communicating to a broader audience with regard to research projects financed with public funds. Scope ● Bionics and biological cybernetics: implantology; bio–abio interfaces ● Bioelectronics: wearable electronics; implantable electronics; “more than Moore” electronics; bioelectronics devices ● Bioprocess and biosystems engineering and applications: bioprocess design; biocatalysis; bioseparation and bioreactors; bioinformatics; bioenergy; etc. ● Biomolecular, cellular and tissue engineering and applications: tissue engineering; chromosome engineering; embryo engineering; cellular, molecular and synthetic biology; metabolic engineering; bio-nanotechnology; micro/nano technologies; genetic engineering; transgenic technology ● Biomedical engineering and applications: biomechatronics; biomedical electronics; biomechanics; biomaterials; biomimetics; biomedical diagnostics; biomedical therapy; biomedical devices; sensors and circuits; biomedical imaging and medical information systems; implants and regenerative medicine; neurotechnology; clinical engineering; rehabilitation engineering ● Biochemical engineering and applications: metabolic pathway engineering; modeling and simulation ● Translational bioengineering
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