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一种新的捕鸟蛛毒素在重组杆状病毒感染期间体外表达时,通过坏死作用导致早期昆虫细胞死亡。

A new theraphosid spider toxin causes early insect cell death by necrosis when expressed in vitro during recombinant baculovirus infection.

作者信息

Ardisson-Araújo Daniel Mendes Pereira, Morgado Fabrício Da Silva, Schwartz Elisabeth Ferroni, Corzo Gerardo, Ribeiro Bergmann Morais

机构信息

Departmento de Biologia Celular, Universidade de Brasília, Brasília, Brasília, DF, Brazil.

Departmento de Ciêncais Fisiológicas, Universidade de Brasília, Brasília, DF, Brazil.

出版信息

PLoS One. 2013 Dec 13;8(12):e84404. doi: 10.1371/journal.pone.0084404. eCollection 2013.

Abstract

Baculoviruses are the most studied insect viruses in the world and are used for biological control of agricultural and forest insect pests. They are also used as versatile vectors for expression of heterologous proteins. One of the major problems of their use as biopesticides is their slow speed to kill insects. Thus, to address this shortcoming, insect-specific neurotoxins from arachnids have been introduced into the baculovirus genome solely aiming to improve its virulence. In this work, an insecticide-like toxin gene was obtained from a cDNA derived from the venom glands of the theraphosid spider Brachypelma albiceps. The mature form of the peptide toxin (called Ba3) has a high content of basic amino acid residues, potential for three possible disulfide bonds, and a predicted three-stranded β-sheetDifferent constructions of the gene were engineered for recombinant baculovirus Autographa californica multiple nuclepolyhedrovirus (AcMNPV) expression. Five different forms of Ba3 were assessed; (1) the full-length sequence, (2) the pro-peptide and mature region, (3) only the mature region, and the mature region fused to an (4) insect or a (5) virus-derived signal peptide were inserted separately into the genome of the baculovirus. All the recombinant viruses induced cell death by necrosis earlier in infection relative to a control virus lacking the toxin gene. However, the recombinant virus containing the mature portion of the toxin gene induced a faster cell death than the other recombinants. We found that the toxin construct with the signal peptide and/or pro-peptide regions delayed the necrosis phenotype. When infected cells were subjected to ultrastructural analysis, the cells showed loss of plasma membrane integrity and structural changes in mitochondria before death. Our results suggest this use of baculovirus is a potential tool to help understand or to identify the effect of insect-specific toxic peptides when produced during infection of insect cells.

摘要

杆状病毒是世界上研究最多的昆虫病毒,用于农业和森林害虫的生物防治。它们还被用作表达异源蛋白的通用载体。将其用作生物杀虫剂的一个主要问题是其杀死昆虫的速度较慢。因此,为了解决这一缺点,已将来自蛛形纲动物的昆虫特异性神经毒素引入杆状病毒基因组, solely aiming to improve its virulence. 在这项工作中,从一种来自白化捕鸟蛛毒液腺的cDNA中获得了一种类似杀虫剂的毒素基因。肽毒素的成熟形式(称为Ba3)具有高含量的碱性氨基酸残基、形成三个可能二硫键的潜力以及预测的三链β-折叠。为杆状病毒苜蓿银纹夜蛾多粒包埋核型多角体病毒(AcMNPV)表达设计了该基因的不同构建体。评估了Ba3的五种不同形式;(1)全长序列,(2)前肽和成熟区域,(3)仅成熟区域,以及与(4)昆虫或(5)病毒衍生信号肽融合的成熟区域分别插入杆状病毒基因组。相对于缺乏毒素基因的对照病毒,所有重组病毒在感染早期通过坏死诱导细胞死亡。然而,含有毒素基因成熟部分的重组病毒比其他重组病毒诱导更快细胞死亡。我们发现带有信号肽和/或前肽区域的毒素构建体延迟了坏死表型。当对感染细胞进行超微结构分析时,细胞在死亡前显示出质膜完整性丧失和线粒体结构变化。我们的结果表明,这种杆状病毒的用途是一种潜在工具,有助于理解或识别昆虫特异性毒性肽在昆虫细胞感染期间产生时的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9f3/3862797/23ff73d884a3/pone.0084404.g001.jpg

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