首页> 外文期刊>Virus Research: An International Journal of Molecular and Cellular Virology >Identification and characterization of a porcine monocytic cell line supporting porcine reproductive and respiratory syndrome virus (PRRSV) replication and progeny virion production by using an improved DNA-launched PRRSV reverse genetics system.
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Identification and characterization of a porcine monocytic cell line supporting porcine reproductive and respiratory syndrome virus (PRRSV) replication and progeny virion production by using an improved DNA-launched PRRSV reverse genetics system.

机译:通过使用改进的DNA发射的PRRSV反向遗传学系统,鉴定和表征支持猪繁殖与呼吸综合征病毒(PRRSV)复制和子代病毒体生产的猪单核细胞系。

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In this study, an improved DNA-launched (plasmid DNA transfection-based) reverse genetics system with reduced cost and labor was developed for porcine reproductive and respiratory syndrome virus (PRRSV) by introduction of ribozyme elements at both termini of the viral genomic cDNA that were placed under the control of a eukaryotic hybrid promoter. The rescue efficacy of PRRSV with this system was approximately 10-50-fold higher than the in vitro-transcribed RNA-based system and the traditional DNA-launched system without the engineered ribozyme elements, as determined by reporter GFP level in transfected cells and the peak titer of the recovery virus. By using this new reverse genetics system, we identified and characterized a porcine monocytic cell line, 3D4/31, capable of supporting PRRSV replication, progeny virion production, and attachment on the cell surface. The establishment of this improved reverse genetic system and the identification of a porcine monocytic cell line supporting PRRSV replication will aid future studies of host-virus interaction of PRRSV.
机译:在这项研究中,通过在病毒基因组cDNA的两个末端引入核酶元件,开发了一种改进的DNA发射(基于质粒DNA转染的)反向遗传系统,该系统具有较低的成本和劳动力,可用于猪繁殖与呼吸综合征病毒(PRRSV)将它们置于真核杂交启动子的控制下。 PRRSV的挽救功效比通过体外转录的基于RNA的体系和不含工程核酶成分的传统DNA发射体系大约高10-50倍,这是由转染细胞和细胞中报道基因GFP的水平确定的。恢复病毒的最高滴度。通过使用这种新的反向遗传学系统,我们鉴定并鉴定了能够支持PRRSV复制,子代病毒体生产以及在细胞表面附着的猪单核细胞系3D4 / 31。建立改进的反向遗传系统并鉴定支持PRRSV复制的猪单核细胞系将有助于PRRSV宿主病毒相互作用的进一步研究。

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