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用于病毒出血性败血病病毒大湖株的反向遗传学系统:NV 基因是致病性所必需的。

A reverse genetics system for the Great Lakes strain of viral hemorrhagic septicemia virus: the NV gene is required for pathogenicity.

机构信息

Center of Marine Biotechnology, University of Maryland Biotechnology Institute, Baltimore, 701 East Pratt Street, Baltimore, MD, 21202-3101, USA.

出版信息

Mar Biotechnol (NY). 2011 Aug;13(4):672-83. doi: 10.1007/s10126-010-9329-4. Epub 2010 Oct 9.

Abstract

Viral hemorrhagic septicemia virus (VHSV), belonging to the genus Novirhabdovirus in the family of Rhabdoviridae, causes a highly contagious disease of fresh and saltwater fish worldwide. Recently, a novel genotype of VHSV, designated IVb, has invaded the Great Lakes in North America, causing large-scale epidemics in wild fish. An efficient reverse genetics system was developed to generate a recombinant VHSV of genotype IVb from cloned cDNA. The recombinant VHSV (rVHSV) was comparable to the parental wild-type strain both in vitro and in vivo, causing high mortality in yellow perch (Perca flavescens). A modified recombinant VHSV was generated in which the NV gene was substituted with an enhanced green fluorescent protein gene (rVHSV-ΔNV-EGFP), and another recombinant was made by inserting the EGFP gene into the full-length viral clone between the P and M genes (rVHSV-EGFP). The in vitro replication kinetics of rVHSV-EGFP was similar to rVHSV; however, the rVHSV-ΔNV-EGFP grew 2 logs lower. In yellow perch challenges, wtVHSV and rVHSV induced 82-100% cumulative per cent mortality (CPM), respectively, whereas rVHSV-EGFP produced 62% CPM and rVHSV-ΔNV-EGFP caused only 15% CPM. No reversion of mutation was detected in the recovered viruses and the recombinant viruses stably maintained the foreign gene after several passages. These results indicate that the NV gene of VHSV is not essential for viral replication in vitro and in vivo, but it plays an important role in viral replication efficiency and pathogenicity. This system will facilitate studies of VHSV replication, virulence, and production of viral vectored vaccines.

摘要

病毒性出血性败血症病毒(VHSV)属于 Rhabdoviridae 科的 Novirhabdovirus 属,可引起全球淡水和海水鱼类的高度传染性疾病。最近,一种新型 VHSV 基因型,称为 IVb,已入侵北美的五大湖,导致野生鱼类大规模爆发疫情。建立了一种有效的反向遗传系统,从克隆 cDNA 中生成 IVb 基因型的重组 VHSV。重组 VHSV(rVHSV)在体外和体内与亲本野生型毒株相当,导致黄鲈(Perca flavescens)高死亡率。生成了一种改良的重组 VHSV,其中 NV 基因被增强型绿色荧光蛋白基因(rVHSV-ΔNV-EGFP)取代,另一种重组病毒是通过在 P 和 M 基因之间的全长病毒克隆中插入 EGFP 基因(rVHSV-EGFP)制成的。rVHSV-EGFP 的体外复制动力学与 rVHSV 相似;然而,rVHSV-ΔNV-EGFP 的生长速度低 2 个对数级。在黄鲈攻毒实验中,wtVHSV 和 rVHSV 分别诱导 82-100%的累积死亡率(CPM),而 rVHSV-EGFP 产生 62%的 CPM,rVHSV-ΔNV-EGFP 仅引起 15%的 CPM。在回收的病毒中未检测到突变的回复,重组病毒在多次传代后仍稳定地维持外源基因。这些结果表明,VHSV 的 NV 基因对于病毒在体外和体内的复制不是必需的,但它在病毒复制效率和致病性中发挥重要作用。该系统将有助于 VHSV 复制、毒力和病毒载体疫苗的研究。

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