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Effective suppression of Dengue virus using a novel group-I intron that induces apoptotic cell death upon infection through conditional expression of the Bax C-terminal domain

机译:使用新型I类内含子有效感染登革热病毒该感染子通过Bax C末端域的条件表达诱导感染后凋亡细胞死亡

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摘要

IntroductionApproximately 100 million confirmed infections and 20,000 deaths are caused by Dengue virus (DENV) outbreaks annually. Global warming and rapid dispersal have resulted in DENV epidemics in formally non-endemic regions. Currently no consistently effective preventive measures for DENV exist, prompting development of transgenic and paratransgenic vector control approaches. Production of transgenic mosquitoes refractory for virus infection and/or transmission is contingent upon defining antiviral genes that have low probability for allowing escape mutations, and are equally effective against multiple serotypes. Previously we demonstrated the effectiveness of an anti-viral group I intron targeting U143 of the DENV genome in mediating trans-splicing and expression of a marker gene with the capsid coding domain. In this report we examine the effectiveness of coupling expression of ΔN Bax to trans-splicing U143 intron activity as a means of suppressing DENV infection of mosquito cells.
机译:简介每年约有1亿例确诊感染病例和2万例死亡是由登革热病毒(DENV)爆发引起的。全球变暖和迅速扩散已导致DENV在正式非流行地区流行。目前尚无针对DENV的始终有效的预防措施,从而促进了转基因和转基因载体控制方法的发展。因病毒感染和/或传播而难治的转基因蚊子的产生取决于确定的抗病毒基因,这些基因的逃逸突变可能性低,并且对多种血清型同样有效。以前,我们证明了靶向DENV基因组U143的抗病毒I组内含子在介导衣壳编码域标记基因的反式剪接和表达中的有效性。在本报告中,我们研究了将ΔNBax的表达与反分裂U143内含子活性偶联作为抑制DENV感染蚊子细胞的有效性。

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