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Towards Bioengineered Liver Stem Cell Transplantation Studies in a Preclinical Dog Model for Inherited Copper Toxicosis

机译:朝向生物工程肝脏干细胞移植研究临床型型铜毒物型临床模型

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摘要

Wilson Disease is a rare autosomal recessive liver disorder in humans. Although its clinical presentation and age of onset are highly variable, hallmarks include signs of liver disease, neurological features and so-called Kayser-Fleischer rings in the eyes of the patient. Hepatic copper accumulation leads to liver disease and eventually to liver cirrhosis. Treatment options include life-long copper chelation therapy and/or decrease in copper intake. Eventually liver transplantations are indicated. Although clinical outcome of liver transplantations is favorable, the lack of suitable donor livers hampers large numbers of transplantations. As an alternative, cell therapies with hepatocytes or liver stem cells are currently under investigation. Stem cell biology in relation to pets is in its infancy. Due to the specific population structure of dogs, canine copper toxicosis is frequently encountered in various dog breeds. Since the histology and clinical presentation resemble Wilson Disease, we combined genetics, gene-editing, and matrices-based stem cell cultures to develop a translational preclinical transplantation model for inherited copper toxicosis in dogs. Here we describe the roadmap followed, starting from the discovery of a causative copper toxicosis mutation in a specific dog breed and culminating in transplantation of genetically-engineered autologous liver stem cells.
机译:威尔逊疾病是人类稀有的常血糖性隐性肝病。虽然其临床介绍和发病年龄是高度变化的,但是标志性包括肝脏疾病的迹象,神经功能和所谓的患者眼中的Kayser-Fleischer环。肝脏铜积聚导致肝病,最终导致肝硬化。治疗方案包括终铜螯合疗法和/或铜摄入量减少。最终显示肝移植。虽然肝移植的临床结果有利,但缺乏合适的供体肝脏阻碍了大量的移植。作为替代方案,目前正在研究具有肝细胞或肝脏干细胞的细胞疗法。与宠物相关的干细胞生物学在其初期。由于狗的特定人口结构,各种狗品种经常遇到犬毒性毒性。由于组织学和临床介绍类似于威尔逊疾病,我们组合遗传学,基因编辑和基于基质的干细胞培养物,为血液中遗传铜毒毒性的平移临床前移植模型。在这里,我们描述了路线图,从发现的特定狗品种中的致病铜毒物突变开始,从遗传工程自体肝干细胞移植中的发现开始。

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