使用黄素单核苷酸(FMN)实时评估HOPE期间同种异体肾移植-一项临床前研究

R. X. Sousa Da Silva, T. Darius, Leandro Mancina, J. Eden, Kendra Wernlé, Ahmed S. Ghoneima, A. Barlow, P. Clavien, P. Dutkowski, P. Kron
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Recently, the release of mitochondria derived fragments, i.e., flavin mononucleotide (FMN) of complex I during machine liver perfusion was shown to be predictive for liver graft function before implantation. Therefore, the aim of this study was to evaluate, if FMN is useful also for assessment of kidney injury before use. Methods A porcine perfusion model was used to investigate the feasibility of assessment of kidney grafts during hypothermic oxygenated perfusion (HOPE) with either 0, 30 or 60 minutes of warm ischemia. The model with warm ischemia times (WIT) of 30 min and 60 min, was used to mimic a clinically relevant scenario. A group with no warm ischemia time (0′ WIT) served as control group. The groups underwent minimal static cold storage (SCS) of 2 h followed by 2 h of end-ischemic HOPE with repeated real-time FMN measurements. 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引用次数: 3

摘要

可用的供体移植和等待名单上的患者之间的差距不断扩大。这导致高风险的肾脏移植的使用增加,因此更容易受到伤害。高风险器官的使用需要在移植前进一步优化机器保存和评估策略。低温机器灌注(HMP)是循环死亡(DCD)后捐赠肾脏的标准护理方法,而低温机器灌注加额外氧气(HOPE)的证据仍然非常有限。此外,缺乏对hmp灌注肾脏的客观质量评估。最近,在机器肝脏灌注过程中,线粒体衍生片段,即复合体I的黄素单核苷酸(FMN)的释放被证明可以预测移植前的肝移植功能。因此,本研究的目的是评估FMN在使用前是否也可用于评估肾损伤。方法采用猪灌注模型,研究在0、30、60分钟热缺血条件下评估移植肾低温氧灌注(HOPE)的可行性。采用热缺血时间(WIT)分别为30 min和60 min的模型模拟临床相关情景。无热缺血时间(0 ' WIT)组作为对照组。各组进行2小时的最小静态冷藏(SCS),然后进行2小时的终末缺血HOPE,并重复实时FMN测量。在进一步的研究中,这些值与损伤相关分子模式(DAMPs)的释放和呼吸链的功能(以ATP产生能力为代表)有关。结果我们首先证明了灌注肾FMN测量的可行性,其次证明了其与供体热缺血时间的相关性。因此,FMN测量结果显示,与30分钟注射组(n = 4)和对照组(n = 4)相比,60分钟注射组(n = 4)的FMN释放量明显更高。FMN的释放也与DAMP信号相关,如8-OHdG和HMGB1的释放。最后,正常肾脏的ATP补充最好,其次是30 min的肾脏,然后是60 min的肾脏。本研究证明了HOPE期间肾脏FMN测量的可行性。此外,我们还显示了FMN定量与先前存在的肾移植损伤之间的相关性。基于此,HOPE期间实时FMN测量可能是接受高危肾移植的客观评估工具,同时最大限度地减少移植后功能障碍,从以前的“直觉”转向接受边缘肾移植的客观标准。基于这些结果的移植物评估可以通过提高利用率来缩小可用移植物和等待名单上的患者之间的差距,而不会对受者产生重大影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Real-time assessment of kidney allografts during HOPE using flavin mononucleotide (FMN) — a preclinical study
Introduction The gap between available donor grafts and patients on the waiting lists is constantly growing. This leads to an increased utilization of high-risk and therefore more vulnerable kidney grafts. The use of high-risk organs requires further optimization of machine preservation and assessment strategies before transplantation. Hypothermic machine perfusion (HMP) is the standard of care for kidneys originating from donation after circulatory death (DCD), whereas the evidence of HMP with additional oxygen (HOPE) is still very limited. Furthermore, an objective quality assessment of HMP-perfused kidneys is lacking. Recently, the release of mitochondria derived fragments, i.e., flavin mononucleotide (FMN) of complex I during machine liver perfusion was shown to be predictive for liver graft function before implantation. Therefore, the aim of this study was to evaluate, if FMN is useful also for assessment of kidney injury before use. Methods A porcine perfusion model was used to investigate the feasibility of assessment of kidney grafts during hypothermic oxygenated perfusion (HOPE) with either 0, 30 or 60 minutes of warm ischemia. The model with warm ischemia times (WIT) of 30 min and 60 min, was used to mimic a clinically relevant scenario. A group with no warm ischemia time (0′ WIT) served as control group. The groups underwent minimal static cold storage (SCS) of 2 h followed by 2 h of end-ischemic HOPE with repeated real-time FMN measurements. In a further step, these values were related to the release of damage-associated molecular patterns (DAMPs) and to the functionality of the respiratory chain, represented by the capacity of ATP production. Results We demonstrate, first, feasibility of perfusate FMN measurements in perfused kidneys, and secondly its correlation with donor warm ischemia time. Accordingly, FMN measurement showed significantly higher release in the 60-minute WIT group (n = 4) compared to the 30-minute WIT (n = 4) and the control group (n = 4). FMN release correlated also with DAMP signaling, such as the release of 8-OHdG and HMGB1. Finally, ATP replenishment proved to be best in control kidneys, followed by kidneys with 30 min and then by kidneys with 60 min of WIT. Discussion This study demonstrates the feasibility of FMN measurement in kidneys during HOPE. In addition, we show a correlation between FMN quantification and pre-existing kidney graft injury. Based on this, real-time FMN measurement during HOPE may be an objective assessment tool to accept high-risk kidneys for transplantation while minimizing post-transplant dysfunction, moving away from former “gut feeling” towards objective criteria in accepting marginal kidney grafts for transplantation. Graft evaluation based on these results may close the gap between available grafts and patients on the waiting lists by increasing utilization rates without significant impact for the recipients.
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