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具有降低细胞毒性和温度敏感性的新型塞姆利基森林病毒载体,用于长期增强转基因表达。

Novel Semliki Forest virus vectors with reduced cytotoxicity and temperature sensitivity for long-term enhancement of transgene expression.

作者信息

Lundstrom Kenneth, Abenavoli Alessandra, Malgaroli Antonio, Ehrengruber Markus U

机构信息

Regulon Inc., Biopole Epalinges, Les Croisettes 22, CH-1066 Epalinges, Switzerland.

出版信息

Mol Ther. 2003 Feb;7(2):202-9. doi: 10.1016/s1525-0016(02)00056-4.

Abstract

Alphaviral vectors inhibit host cell protein synthesis and are cytotoxic. To overcome these limitations, we modified the nonstructural protein-2 (nsP2) gene in the Semliki Forest virus (SFV) vector, pSFV1. Packaging of SFV replicons with two point mutations in nsP2 resulted in high-titer recombinant SFV(PD) particles. SFV(PD) led to more efficient host cell protein synthesis, exhibited reduced cytotoxicity and improved cell survival, and allowed greater and prolonged transgene expression than the original vector, SFV. In dissociated hippocampal neurons and organotypic rat hippocampal slices, SFV(PD) infection preserved neuronal morphology and synaptic function more efficiently than SFV. Combination of the two point mutations with a replication-persistent mutation in nsP2 resulted in a highly temperature-sensitive vector, SFV(PD713P), which efficiently transduced neurons in hippocampal slice cultures. At 31 degrees C, SFV(PD713P) allowed continuous transgene expression in BHK cells, at amounts comparable to SFV(PD). These new SFV mutants are expected to substantially broaden the application of alphaviral vectors in neurons and other mammalian cells.

摘要

甲病毒载体可抑制宿主细胞蛋白质合成,具有细胞毒性。为克服这些局限性,我们对辛德毕斯病毒(SFV)载体pSFV1中的非结构蛋白2(nsP2)基因进行了修饰。对nsP2具有两个点突变的SFV复制子进行包装,产生了高滴度的重组SFV(PD)颗粒。与原始载体SFV相比,SFV(PD)能更有效地促进宿主细胞蛋白质合成,细胞毒性降低,细胞存活率提高,且能实现更高水平和更长时间的转基因表达。在解离的海马神经元和大鼠海马脑片培养物中,SFV(PD)感染比SFV更有效地维持了神经元形态和突触功能。将这两个点突变与nsP2中的一个复制持续性突变相结合,产生了一种高度温度敏感的载体SFV(PD713P),它能有效地转导海马脑片培养物中的神经元。在31摄氏度时,SFV(PD713P)能在BHK细胞中持续表达转基因,表达量与SFV(PD)相当。这些新的SFV突变体有望显著拓宽甲病毒载体在神经元和其他哺乳动物细胞中的应用。

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