细胞疗法去除威尔逊病中的多余铜。
Cell therapy to remove excess copper in Wilson's disease.
机构信息
Marion Bessin Liver Research Center, Cancer Research Center, Diabetes Center, Departments of Medicine and Pathology, Ruth L. and David S. Gottesman Institute for Stem Cell and Regenerative Medicine Research, and Institute for Clinical and Translational Research, Albert Einstein College of Medicine, Bronx, New York.
出版信息
Ann N Y Acad Sci. 2014 May;1315(1):70-80. doi: 10.1111/nyas.12450.
To achieve permanent correction of Wilson's disease by a cell therapy approach, replacement of diseased hepatocytes with healthy hepatocytes is desirable. There is a physiological requirement for hepatic ATP7B-dependent copper (Cu) transport in bile, which is deficient in Wilson's disease, producing progressive Cu accumulation in the liver or brain with organ damage. The ability to repopulate the liver with healthy hepatocytes raises the possibility of cell therapy in Wilson's disease. Therapeutic principles included reconstitution of bile canalicular network as well as proliferation in transplanted hepatocytes, despite toxic amounts of Cu in the liver. Nonetheless, cell therapy studies in animal models elicited major differences in the mechanisms driving liver repopulation with transplanted hepatocytes in Wilson's disease versus nondiseased settings. Recently, noninvasive imaging was developed to demonstrate Cu removal from the liver, including after cell therapy in Wilson's disease. Such developments will help advance cell/gene therapy approaches, particularly by offering roadmaps for clinical trials in people with Wilson's disease.
为了通过细胞治疗方法实现威尔逊病的永久矫正,用健康的肝细胞替代患病的肝细胞是理想的。在胆汁中,肝 ATP7B 依赖性铜(Cu)转运存在生理需求,而威尔逊病中该转运是缺乏的,导致肝脏或大脑中的 Cu 不断蓄积,从而发生器官损伤。用健康的肝细胞重新填充肝脏的能力为威尔逊病的细胞治疗提供了可能性。治疗原则包括再形成胆小管网络以及移植的肝细胞增殖,尽管肝脏中含有大量的 Cu。尽管如此,在动物模型中的细胞治疗研究表明,在威尔逊病和非疾病状态下,驱动移植的肝细胞在肝脏中再增殖的机制存在显著差异。最近,开发了非侵入性成像技术来证明从肝脏中去除 Cu,包括在威尔逊病的细胞治疗之后。这些进展将有助于推进细胞/基因治疗方法,特别是为威尔逊病患者的临床试验提供路线图。
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