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Procurement and Evaluation of Hepatocytes for Transplantation From Neonatal Donors After Circulatory Death

机译:循环死亡后新生儿供体移植肝细胞的获取和评价

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摘要

Hepatocyte transplantation is a promising treatment for liver failure and inborn metabolic liver diseases, but progress has been hampered by a scarcity of available organs. Here, hepatocytes isolated from livers procured for a neonatal hepatocyte donation program within a research setting were assessed for metabolic function and suitability for transplantation. Organ donation was considered for infants who died in neonatal intensive care in the Stockholm region during 2015–2021. Inclusion was assessed when a decision to discontinue life-sustaining treatment had been made and hepatectomy performed after declaration of death. Hepatocyte isolation was performed by three-step collagenase perfusion. Hepatocyte viability, yield, and function were assessed using fresh and cryopreserved cells. Engraftment and maturation of cryopreserved neonatal hepatocytes were assessed by transplantation into an immunodeficient mouse model and analysis of the gene expression of phase I, phase II, and liver-specific enzymes and proteins. Twelve livers were procured. Median warm ischemia time (WIT) was 190 [interquartile range (IQR): 80–210] minutes. Median viability was 86% (IQR: 71%–91%). Median yield was 6.9 (IQR: 3.4–12.8) x106 viable hepatocytes/g. Transplantation into immunodeficient mice resulted in good engraftment and maturation of hepatocyte-specific proteins and enzymes. A neonatal organ donation program including preterm born infants was found to be feasible. Hepatocytes isolated from neonatal donors had good viability, function, and engraftment despite prolonged WIT. Therefore, neonatal livers should be considered as a donor source for clinical hepatocyte transplantation, even in cases with extended WIT.
机译:肝细胞移植是治疗肝衰竭和先天性代谢性肝病的一种很有前途的治疗方法,但由于可用器官的稀缺,进展受到了阻碍。在这里,评估了从研究环境中为新生儿肝细胞捐赠计划采购的肝脏中分离的肝细胞的代谢功能和移植适宜性。2015-2021 年期间,斯德哥尔摩地区新生儿重症监护室死亡的婴儿被考虑进行器官捐献。当决定停止维持生命治疗并在宣布死亡后进行肝切除术时,评估纳入。肝细胞分离通过三步胶原酶灌注进行。使用新鲜和冻存细胞评估肝细胞活力、产量和功能。通过移植到免疫缺陷小鼠模型中并分析 I 期、 II 期和肝脏特异性酶和蛋白质的基因表达来评估冷冻保存的新生肝细胞的植入和成熟。采购了 12 个肝脏。中位热缺血时间 (WIT) 为 190 [四分位距 (IQR):80-210] 分钟。中位存活率为 86% (IQR: 71%–91%)。中位产量为 6.9 (IQR: 3.4–12.8) x106 活肝细胞/g。移植到免疫缺陷小鼠中导致肝细胞特异性蛋白和酶的良好植入和成熟。包括早产儿在内的新生儿器官捐献计划被发现是可行的。尽管 WIT 延长,但从新生儿供体中分离的肝细胞具有良好的活力、功能和植入。因此,应将新生儿肝脏视为临床肝细胞移植的供体来源,即使在 WIT 扩展的情况下也是如此。

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