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通过血流动力学控制的 DCD 预防缺血性心肌挛缩。

Prevention of Ischemic Myocardial Contracture Through Hemodynamically Controlled DCD.

机构信息

Department of Automatic Control, Lund University, Lund, Sweden.

Division of Thoracic Surgery, Department of Clinical Sciences, Lund University, Lund, Sweden.

出版信息

Cardiovasc Eng Technol. 2021 Oct;12(5):485-493. doi: 10.1007/s13239-021-00537-8. Epub 2021 Apr 29.

Abstract

PURPOSE

Ischemic myocardial contracture (IMC) or "stone heart" is a condition with rapid onset following circulatory death. It inhibits transplantability of hearts donated upon circulatory death (DCD). We investigate the effectiveness of hemodynamic normalization upon withdrawal of life-sustaining therapy (WLST) in a large-animal controlled DCD model, with the hypothesis that reduction in cardiac work delays the onset of IMC.

METHODS

A large-animal study was conducted comprising of a control group ([Formula: see text]) receiving no therapy upon WLST, and a test group ([Formula: see text]) subjected to a protocol for fully automated computer-controlled hemodynamic drug administration. Onset of IMC within 1 h following circulatory death defined the primary end-point. Cardiac work estimates based on pressure-volume loop concepts were developed and used to provide insight into the effectiveness of the proposed computer-controlled therapy.

RESULTS

No test group individual developed IMC within [Formula: see text], whereas all control group individuals did (4/6 within [Formula: see text]).

CONCLUSION

Automatic dosing of hemodynamic drugs in the controlled DCD context has the potential to prevent onset of IMC up to [Formula: see text], enabling ethical and medically safe organ procurement. This has the potential to increase the use of DCD heart transplantation, which has been widely recognized as a means of meeting the growing demand for donor hearts.

摘要

目的

缺血性心肌挛缩(IMC)或“石心”是一种在循环死亡后迅速发生的疾病。它抑制了循环死亡后捐献的心脏(DCD)的可移植性。我们在大型动物对照 DCD 模型中研究了在停止生命支持治疗(WLST)时进行血液动力学正常化的效果,假设减少心脏做功可延迟 IMC 的发生。

方法

进行了一项大型动物研究,包括对照组([公式:见正文])在 WLST 后不接受任何治疗,以及实验组([公式:见正文])接受完全自动计算机控制的血液动力学药物给药方案。循环死亡后 1 小时内 IMC 的发生定义为主要终点。基于压力-容积环概念开发了心脏做功估计,并用于深入了解所提出的计算机控制治疗的效果。

结果

没有一个实验组个体在[公式:见正文]内发生 IMC,而对照组所有个体均发生了 IMC(4/6 在[公式:见正文]内)。

结论

在对照 DCD 环境中自动给药血液动力学药物有可能预防 IMC 的发生,最长可达[公式:见正文],从而实现符合伦理和医学安全的器官获取。这有可能增加 DCD 心脏移植的使用,这已被广泛认为是满足日益增长的供体心脏需求的一种手段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e224/8481220/b81f1c34d19e/13239_2021_537_Fig1_HTML.jpg

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