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转 基因 斯氏按蚊 共表达 单链抗体 抵抗 恶性疟原虫 发育。

Transgenic Anopheles stephensi coexpressing single-chain antibodies resist Plasmodium falciparum development.

机构信息

Department of Microbiology and Molecular Genetics, School of Medicine, University of California, Irvine, CA 92697-4500, USA.

出版信息

Proc Natl Acad Sci U S A. 2012 Jul 10;109(28):E1922-30. doi: 10.1073/pnas.1207738109. Epub 2012 Jun 11.

Abstract

Anopheles stephensi mosquitoes expressing m1C3, m4B7, or m2A10 single-chain antibodies (scFvs) have significantly lower levels of infection compared to controls when challenged with Plasmodium falciparum, a human malaria pathogen. These scFvs are derived from antibodies specific to a parasite chitinase, the 25 kDa protein and the circumsporozoite protein, respectively. Transgenes comprising m2A10 in combination with either m1C3 or m4B7 were inserted into previously-characterized mosquito chromosomal "docking" sites using site-specific recombination. Transgene expression was evaluated at four different genomic locations and a docking site that permitted tissue- and sex-specific expression was researched further. Fitness studies of docking site and dual scFv transgene strains detected only one significant fitness cost: adult docking-site males displayed a late-onset reduction in survival. The m4B7/m2A10 mosquitoes challenged with P. falciparum had few or no sporozoites, the parasite stage infective to humans, in three of four experiments. No sporozoites were detected in m1C3/m2A10 mosquitoes in challenge experiments when both genes were induced at developmentally relevant times. These studies support the conclusion that expression of a single copy of a dual scFv transgene can completely inhibit parasite development without imposing a fitness cost on the mosquito.

摘要

表达 m1C3、m4B7 或 m2A10 单链抗体 (scFv) 的斯氏按蚊与对照相比,在感染疟原虫时感染水平显著降低,疟原虫是一种人类疟疾病原体。这些 scFv 分别来自针对寄生虫几丁质酶、25kDa 蛋白和环子孢子蛋白的抗体。包含 m2A10 的转基因与 m1C3 或 m4B7 结合,使用位点特异性重组插入到先前表征的蚊子染色体“对接”位点。在四个不同的基因组位置和一个允许组织和性别特异性表达的对接位点评估转基因表达。对接位点和双 scFv 转基因株系的适应度研究仅检测到一个显著的适应度代价:对接位点的成年雄性表现出晚期生存能力降低。在四项实验中的三项中,用疟原虫感染的 m4B7/m2A10 蚊子中几乎没有或没有感染人类的寄生虫阶段——孢子虫。当两个基因在发育相关时间被诱导时,在 m1C3/m2A10 蚊子的挑战实验中未检测到孢子虫。这些研究支持这样的结论,即表达单个双 scFv 转基因拷贝可以完全抑制寄生虫发育,而不会对蚊子造成适应度代价。

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