无创椎管内经皮灌注监测:透过皮肤看心脏。

Frontiers in nephrology Pub Date : 2023-07-11 eCollection Date: 2023-01-01 DOI:10.3389/fneph.2023.1124130
Jarrin D Penny, Lisa Hur, Fabio R Salerno, Dickson Wong, M Hussain Jan, Christopher W McIntyre
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摘要

导言:血液透析(HD)这种维持生命的治疗方法会引起反复和累积性的全身循环压力,导致心血管损伤。这些反复出现的损伤会加重原有的心血管后遗症,导致心肌损伤,并造成极高的发病率/死亡率。这在很大程度上是心肌内微循环流量受到挑战的结果(详细的成像研究证明了这一点)。目前,血液透析过程中的监测是在大血管层面进行的。对器官灌注的无创监测可检测并治疗改善 HD 的这种病理生理反应。对皮肤的非侵入性经皮灌注监测(使用光电血压计-PPG)已被证明可预测 HD 引起的心肌骤停(节段性缺血的结果)。在本研究中,我们扩展了这些观察结果,将血液透析期间皮肤灌注的动态评估与透析期间直接测量的心肌灌注和心脏收缩功能进行了比较:方法:我们在整个血液透析过程中使用连续的经皮血流灌注监测对 12 名接受常规血液透析治疗的患者进行了透析内微循环反应评估。在开始血液透析前进行心脏超声心动图检查,并在血液透析压力峰值时再次进行检查,以评估区域室壁运动异常(RWMA)的发展情况。利用静脉注射的造影剂和基于计算机断层扫描(CT)的方法,在相同的时间点(HD 前和 HD 峰值应激)进行心肌灌注成像。将椎管内脉搏强度的变化(通过 PPG 得出)与 HD 诱导的 RWMAs(表明心肌损伤)和心肌灌注的变化进行比较:结果:我们发现最低脉搏强度下降(PPG)与 RWMAs 的发生(p = 0.03)以及与整体心肌灌注(CT)的变化(p = 0.05)之间存在关联。超滤率(毫升/千克/小时)是血液透析诱发循环压力的重要驱动因素[(与最大脉搏强度降低(p = 0.01)、总体心肌灌注减少(p = 0.001)和 RWMA 的发生(p = 0.03)相关)]:讨论:使用 PPG 进行经皮血流灌注监测是评估椎管内血流动力学稳定性和 HD 诱导的循环压力的有效方法。在皮肤微循环水平产生的信息反映了心肌灌注的直接测量结果以及 HD 诱导的心肌损伤的发展情况。这种检测和处理 HD 引起的心脏损伤的方法值得进一步评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Non-invasive intradialytic percutaneous perfusion monitoring: a view to the heart through the skin.

Introduction: The life-sustaining treatment of hemodialysis (HD) induces recurrent and cumulative systemic circulatory stress resulting in cardiovascular injury. These recurrent insults compound preexisting cardiovascular sequalae leading to the development of myocardial injury and resulting in extremely high morbidity/mortality. This is largely a consequence of challenged microcirculatory flow within the myocardium (evidenced by detailed imaging-based studies). Currently, monitoring during HD is performed at the macrovascular level. Non-invasive monitoring of organ perfusion would allow the detection and therapeutic amelioration of this pathophysiological response to HD. Non-invasive percutaneous perfusion monitoring of the skin (using photoplethysmography-PPG) has been shown to be predictive of HD-induced myocardial stunning (a consequence of segmental ischemia). In this study, we extended these observations to include a dynamic assessment of skin perfusion during HD compared with directly measured myocardial perfusion during dialysis and cardiac contractile function.

Methods: We evaluated the intradialytic microcirculatory response in 12 patients receiving conventional HD treatments using continuous percutaneous perfusion monitoring throughout HD. Cardiac echocardiography was performed prior to the initiation of HD, and again at peak-HD stress, to assess the development of regional wall motion abnormalities (RWMAs). Myocardial perfusion imaging was obtained at the same timepoints (pre-HD and peak-HD stress), utilizing intravenous administered contrast and a computerized tomography (CT)-based method. Intradialytic changes in pulse strength (derived from PPG) were compared with the development of HD-induced RWMAs (indicative of myocardial stunning) and changes in myocardial perfusion.

Results: We found an association between the lowest pulse strength reduction (PPG) and the development of RWMAs (p = 0.03) and also with changes in global myocardial perfusion (CT) (p = 0.05). Ultrafiltration rate (mL/kg/hour) was a significant driver of HD-induced circulatory stress [(associated with the greatest pulse strength reduction (p = 0.01), a reduction in global myocardial perfusion (p = 0.001), and the development of RWMAs (p = 0.03)].

Discussion: Percutaneous perfusion monitoring using PPG is a useful method of assessing intradialytic hemodynamic stability and HD-induced circulatory stress. The information generated at the microcirculatory level of the skin is reflective of direct measures of myocardial perfusion and the development of HD-induced myocardial stunning. This approach for the detection and management of HD-induced cardiac injury warrants additional evaluation.

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Vascular injury in glomerulopathies: the role of the endothelium. Editorial: Insights in glomerular disease. The Janus-faced nature of complement in hemodialysis: interplay between complement, inflammation, and bioincompatibility unveiling a self-amplifying loop contributing to organ damage. Comparative iron management in hemodialysis and peritoneal dialysis patients: a systematic review. Analyzing body composition in living kidney donors: impact on post-transplant kidney function.
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