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通过腺相关病毒基因转移治疗人类疾病。

Treatment of human disease by adeno-associated viral gene transfer.

作者信息

Warrington Kenneth H, Herzog Roland W

机构信息

Cellular and Molecular Therapy, Department of Pediatrics, University of Florida, Gainesville, FL 32615-9586, USA.

出版信息

Hum Genet. 2006 Jul;119(6):571-603. doi: 10.1007/s00439-006-0165-6. Epub 2006 Apr 13.

Abstract

During the past decade, in vivo administration of viral gene transfer vectors for treatment of numerous human diseases has been brought from bench to bedside in the form of clinical trials, mostly aimed at establishing the safety of the protocol. In preclinical studies in animal models of human disease, adeno-associated viral (AAV) vectors have emerged as a favored gene transfer system for this approach. These vectors are derived from a replication-deficient, non-pathogenic parvovirus with a single-stranded DNA genome. Efficient gene transfer to numerous target cells and tissues has been described. AAV is particularly efficient in transduction of non-dividing cells, and the vector genome persists predominantly in episomal forms. Substantial correction, and in some instances complete cure, of genetic disease has been obtained in animal models of hemophilia, lysosomal storage disorders, retinal diseases, disorders of the central nervous system, and other diseases. Therapeutic expression often lasted for months to years. Treatments of genetic disorders, cancer, and other acquired diseases are summarized in this review. Vector development, results in animals, early clinical experience, as well as potential hurdles and challenges are discussed.

摘要

在过去十年中,用于治疗多种人类疾病的病毒基因转移载体的体内给药已通过临床试验的形式从实验室走向临床应用,这些试验大多旨在确立方案的安全性。在人类疾病动物模型的临床前研究中,腺相关病毒(AAV)载体已成为这种方法中备受青睐的基因转移系统。这些载体源自一种复制缺陷型、非致病性的细小病毒,其基因组为单链DNA。已有报道表明,AAV能有效地将基因转移至多种靶细胞和组织。AAV在转导非分裂细胞方面尤为高效,且载体基因组主要以游离形式存在。在血友病、溶酶体贮积症、视网膜疾病、中枢神经系统疾病及其他疾病的动物模型中,已实现了对遗传疾病的显著纠正,在某些情况下甚至实现了完全治愈。治疗性表达通常可持续数月至数年。本文综述了遗传性疾病、癌症及其他后天性疾病的治疗情况。讨论了载体的研发、在动物实验中的结果、早期临床经验以及潜在的障碍与挑战。

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