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在针对致命疾病的基于基因医学的临床研究中,直面治疗误解、入组决策和个人动机等问题。

Confronting the issues of therapeutic misconception, enrollment decisions, and personal motives in genetic medicine-based clinical research studies for fatal disorders.

作者信息

Arkin Lisa M, Sondhi Dolan, Worgall Stefan, Suh Lily Hyon K, Hackett Neil R, Kaminsky Stephen M, Hosain Syed A, Souweidane Mark M, Kaplitt Michael G, Dyke Jonathan P, Heier Linda A, Ballon Douglas J, Shungu Dikoma C, Wisniewski Krystyna E, Greenwald Bruce M, Hollmann Charleen, Crystal Ronald G

机构信息

Department of Genetic Medicine, Weill Medical College of Cornell University, New York, NY 10021, USA.

出版信息

Hum Gene Ther. 2005 Sep;16(9):1028-36. doi: 10.1089/hum.2005.16.1028.

Abstract

Genetic medicine-based therapies have unlocked the potential for ameliorating diseases previously considered inevitably fatal. Inherent in the clinical trials of genetic medicines are ethical issues of therapeutic misconception, enrollment decisions as they relate to the risks and benefits of research, and the complex relationships among funding sources, investigators, and the families of affected individuals. The purpose of this paper is to help define these complex issues relevant to the use of genetic medicines and to describe the strategy we have used to confront these issues in a phase I trial of adeno-associated virus-mediated gene transfer to the central nervous system of children with late infantile neuronal ceroid lipofuscinosis (LINCL), a fatal lysosomal storage disease associated with progressive neurodegeneration and death by mid-childhood. Our approach to these challenges should provide a useful paradigm for investigators initiating other genetic medicine- based studies to treat inevitably fatal diseases.

摘要

基于基因医学的疗法已开启了改善以往被认为不可避免会致命的疾病的可能性。基因药物临床试验中存在一些伦理问题,如治疗误解、与研究风险和益处相关的入组决策,以及资金来源、研究者和受影响个体家庭之间的复杂关系。本文旨在帮助界定与基因药物使用相关的这些复杂问题,并描述我们在一项针对晚发性婴儿神经元蜡样脂褐质沉积症(LINCL)患儿中枢神经系统进行腺相关病毒介导的基因转移的I期试验中用以应对这些问题的策略。LINCL是一种致命的溶酶体贮积病,与进行性神经退行性变相关,患儿到童年中期会死亡。我们应对这些挑战的方法应为开展其他基于基因医学的研究以治疗不可避免会致命的疾病的研究者提供一个有用的范例。

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