Pediatric Liver GI and Nutrition Centre and Mowat Labs, King's College Hospital, London, United Kingdom.
King's College London, London, United Kingdom.
PLoS One. 2023 Jul 25;18(7):e0288185. doi: 10.1371/journal.pone.0288185. eCollection 2023.
Pediatric acute liver failure (PALF) carries a high mortality without liver transplantation (LT) in children. Liver transplantation, though lifesaving, is limited by timely donor organ availability, the risks of major surgery and complications of life-long immunosuppression. Hepatocyte transplantation (HT) improves synthetic and detoxification functions in small animal models. The encapsulation of hepatocytes in alginate protects it from the recipient immune system while the intraperitoneal route of administration allows large volumes to be infused. The safety and possibly short-term efficacy of encapsulated hepatocytes has been observed in a named patient use. A novel type of microbeads (HMB002) has been developed, using a modified alginate and mesenchymal stromal cells (MSCs). Its safety and medium-term efficacy need to be studied in the context of clinical study while optimizing the hepatocyte function and viability using modifications of the alginate and MSCs co-encapsulation.
A single centre, non-randomised, open-label, single-arm Simon's two stage study will be conducted to evaluate the safety, biological activity and tolerability of transplantation of a single intraperitoneal dose of microbeads made from an optimum combination of a modified alginate, MSCs and hepatocytes in 17 patients less than 16 years of age with acute liver failure (Stage 1: 9 patients and Stage 2: 8 patient). Safety will be assessed by documenting moderate to severe (including life threatening and death) adverse events due to HMB002 in the first 52 weeks post-procedure. Tolerability will be assessed by observing the proportion of initiated infusions where >80% of infusion is received by the patient. Biological activity will be reflected in patient survival with native liver at 24 weeks post treatment.
HMB002, if safe and efficacious in acute liver failure, could be a bridge until the liver regenerates or a suitable organ becomes available. There are multiple advantages to using HT. HT, when delivered by the intraperitoneal route, is less invasive than LT. Hepatocytes from a single donor liver can be used to treat multiple patients. Cryopreserved cells provide an off-the-shelf emergency treatment in PALF. When encapsulated, alginate encapsulation of hepatocytes precludes the need for immunosuppression unlike in LT.
小儿急性肝衰竭(PALF)如果不进行肝移植(LT),死亡率很高。尽管 LT 可以救命,但由于及时获得供体器官的限制、大手术的风险以及长期免疫抑制的并发症,其应用受到限制。肝细胞移植(HT)可改善小动物模型的合成和解毒功能。藻酸盐包裹的肝细胞可防止其被受者免疫系统破坏,而腹腔内给药途径可使大量肝细胞被注入。在一名指定患者的使用中观察到包裹的肝细胞的安全性和可能的短期疗效。已经开发出一种新型微球(HMB002),使用改良的藻酸盐和间充质基质细胞(MSCs)。在临床研究中,需要研究其安全性和中期疗效,同时通过改良藻酸盐和 MSC 共包封来优化肝细胞的功能和活力。
将进行一项单中心、非随机、开放标签、单臂 Simon 两阶段研究,以评估在 17 名年龄小于 16 岁的急性肝衰竭患者(第 1 阶段:9 名患者和第 2 阶段:8 名患者)中单次腹腔内给予最佳组合的改良藻酸盐、MSCs 和肝细胞制成的微球的单次剂量的安全性、生物活性和耐受性。安全性将通过记录手术后 52 周内因 HMB002 导致的中度至重度(包括危及生命和死亡)不良事件来评估。耐受性将通过观察接受>80%输注的启动输注比例来评估。生物活性将反映在治疗后 24 周时患者的存活情况。
如果 HMB002 在急性肝衰竭中安全且有效,则可以作为等待肝脏再生或获得合适器官的桥梁。使用 HT 有多个优势。当通过腹腔内途径给药时,HT 比 LT 侵入性更小。来自单个供体肝脏的肝细胞可用于治疗多个患者。冷冻保存的细胞为 PALF 提供了紧急治疗的现货。与 LT 不同,当用藻酸盐包裹时,包裹的肝细胞不需要免疫抑制。
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