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[自我互补腺相关病毒载体的发展趋势]

[Trends in development of self-complementary adeno-associated virus vector].

作者信息

Lü Yinghui, Wang Qizhao, Xiao Weidong, Diao Yong, Xu Rui'an

机构信息

Institute of Molecular Medicine, Huaqiao University, Fujian 362021, China.

出版信息

Sheng Wu Gong Cheng Xue Bao. 2009 May;25(5):658-64.

Abstract

Numerous studies and clinical trials have demonstrated the efficacy of recombinant adeno-associated virus gene delivery vectors. However, prior to expression, it is necessary to convert the single-stranded DNA genome into double-stranded DNA, which hinders the efficiency of these vectors. We can entirely circumvent this step through the use of self-complementary recombinant adeno-associated virus vector (scrAAV). ScrAAV packages an inverted repeat genome that can fold into double-stranded DNA without the requirement for DNA synthesis or base-pairing between multiple vector genomes. By using scrAAV, we could increase expression efficiency and reduce immune response caused by vectors themselves. Therefore, it is a promising vector for gene therapy. So far, it has been used in the treatment of hepatic diseases, central nervous system diseases, and eye diseases. It has also been used in the modifications of stem cells and as vectors for siRNA/miRNA and ribozymes. In this review, we focused on the preparation, expression and location of scrAAV both in vitro and in vivo. We mainly introduced the recent progress of scrAAV based therapy of Hemophilia B, in order to elucidate the potential and prospects of scrAAV in gene therapy.

摘要

大量的研究和临床试验已经证明了重组腺相关病毒基因递送载体的有效性。然而,在表达之前,有必要将单链DNA基因组转化为双链DNA,这阻碍了这些载体的效率。我们可以通过使用自我互补重组腺相关病毒载体(scrAAV)完全规避这一步骤。ScrAAV包装了一个反向重复基因组,该基因组可以折叠成双链DNA,而无需DNA合成或多个载体基因组之间的碱基配对。通过使用scrAAV,我们可以提高表达效率并减少载体本身引起的免疫反应。因此,它是一种很有前途的基因治疗载体。到目前为止,它已被用于治疗肝脏疾病、中枢神经系统疾病和眼部疾病。它也被用于干细胞的修饰以及作为siRNA/miRNA和核酶的载体。在这篇综述中,我们重点关注了scrAAV在体外和体内的制备、表达和定位。我们主要介绍了基于scrAAV的B型血友病治疗的最新进展,以阐明scrAAV在基因治疗中的潜力和前景。

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