Transmission from the vertebrate host to the mosquito vector represents a major population bottleneck in the malaria life cycle that can successfully be targeted by intervention strategies. However, to date only about 25 parasite proteins expressed during this critical phase have been functionally analysed by gene disruption. We describe the first systematic, larger scale generation and phenotypic analysis of Plasmodium berghei knockout (KO) lines, characterizing 20 genes encoding putatively secreted proteins expressed by the ookinete, the parasite stage responsible for invasion of the mosquito midgut. Of 12 KO lines that were generated, six showed significant reductions in parasite numbers during development in the mosquito, resulting in a block in transmission of five KOs. While expression data, time point of essential function and mutant phenotype correlate well in three KOs defective in midgut invasion, in three KOs that fail at sporulation, maternal inheritance of the mutant phenotype suggests that essential function occurs during ookinete formation and thus precedes morphological abnormalities by several days.

译文

从脊椎动物宿主到蚊子媒介的传播代表了疟疾生命周期中的主要人口瓶颈,可以通过干预策略成功地将其作为目标。然而,迄今为止,仅通过基因破坏对在此关键阶段表达的约25种寄生虫蛋白进行了功能分析。我们描述了伯氏疟原虫敲除 (KO) 系的首次系统,较大规模的生成和表型分析,表征了20个基因,这些基因编码由卵代表达的推测分泌的蛋白质,这是负责蚊子中肠入侵的寄生虫阶段。在产生的12个KO品系中,有6个在蚊子发育过程中寄生虫数量显着减少,导致5个KO的传播受到阻碍。虽然表达数据,基本功能的时间点和突变表型在中肠入侵有缺陷的三个KOs中具有良好的相关性,在三个在孢子形成时失败的KOs中,突变表型的母体遗传表明基本功能发生在卵代发育过程中,因此先于形态异常几天。

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