首页> 外文期刊>Human gene therapy >Unique characteristics of AAV1, 2, and 5 viral entry, intracellular trafficking, and nuclear import define transduction efficiency in HeLa cells.
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Unique characteristics of AAV1, 2, and 5 viral entry, intracellular trafficking, and nuclear import define transduction efficiency in HeLa cells.

机译:AAV1、2和5病毒进入,细胞内运输和核输入的独特特征定义了HeLa细胞的转导效率。

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Biological differences between recombinant adeno-associated virus (rAAV) serotypes define their efficiencies in expressing a transgene in a particular target cell. Few studies have directly compared how differences in viral entry, intracellular trafficking, and nuclear import of rAAV serotypes influence the effectiveness of transduction in the same cell type. We evaluated these characteristics for three rAAV serotypes in HeLa cells, using biochemical techniques and fluorescence-based detection of multiple serotypes in the same cell. Although rAAV2 exhibited the slowest entry, intracellular trafficking, and nuclear import among the three serotypes, it elicited the highest levels of transduction. Conversely, rAAV1 exhibited more rapid entry and nuclear import than the other serotypes, yet was ineffective at transducing HeLa cells due to impaired capsid disassembly in the nucleus. rAAV5, which entered the cell less rapidly than rAAV1, was imported efficiently into the nucleus, but then rapidly degraded, resulting in poor transduction of HeLa cells. We conclude that rAAV1, 2, and 5 utilize distinct mechanisms for intracellular trafficking, and that post-nuclear events play an important role in determining the efficiency of HeLa cell transduction by these serotypes. Thus, overcoming post-nuclear barriers that limit uncoating and/or promote virion degradation may enhance the efficiency of certain AAV serotypes.
机译:重组腺相关病毒(rAAV)血清型之间的生物学差异定义了它们在特定靶细胞中表达转基因的效率。很少有研究直接比较病毒进入,细胞内运输和rAAV血清型的核输入差异如何影响同一细胞类型中转导的有效性。我们使用生物化学技术和基于荧光的同一细胞中多种血清型检测,评估了HeLa细胞中三种rAAV血清型的这些特征。尽管rAAV2在这三种血清型中表现出最慢的进入,细胞内运输和核输入,但它引发了最高水平的转导。相反,rAAV1比其他血清型表现出更快的进入和核输入,但是由于核中衣壳的分解受损,在转导HeLa细胞方面无效。 rAAV5进入细胞的速度比rAAV1慢,但被有效导入细胞核,但随后迅速降解,导致HeLa细胞转导不良。我们得出的结论是,rAAV1、2和5利用不同的机制进行细胞内运输,并且核后事件在确定这些血清型转导HeLa细胞的效率中起重要作用。因此,克服限制脱膜和/或促进病毒体降解的核后屏障可以提高某些AAV血清型的效率。

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