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首页> 外文期刊>mSphere >Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants
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Phenotypic Screens Identify Parasite Genetic Factors Associated with Malarial Fever Response in Plasmodium falciparum piggyBac Mutants

机译:表型筛选确定与恶性疟原虫piggyBac突变体中的疟疾反应相关的寄生虫遗传因素。

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Malaria remains one of the most devastating parasitic diseases worldwide, with 90% of the malaria deaths in Africa in 2013 attributable to Plasmodium falciparum . The clinical symptoms of malaria include cycles of fever, corresponding to parasite rupture from red blood cells every 48?h. Parasite pathways involved in the parasite’s ability to survive the host fever response, and indeed, the functions of ~40% of P.?falciparum genes as a whole, are still largely unknown. Here, we evaluated the potential of scalable forward-genetic screening methods to identify genes involved in the host fever response. We performed a phenotypic screen for genes linked to the parasite response to febrile temperatures by utilizing a selection of single-disruption P.?falciparum mutants generated via random piggyBac transposon mutagenesis in a previous study. We identified several mutants presenting significant phenotypes in febrile response screens compared to the wild type, indicating possible roles for the disrupted genes in this process. We present these initial studies as proof that forward genetics can be used to gain insight into critical factors associated with parasite biology. IMPORTANCE Though the P.?falciparum genome sequence has been available for many years, ~40% of its genes do not have informative annotations, as they show no detectable homology to those of studied organisms. More still have not been evaluated via genetic methods. Scalable forward-genetic approaches that allow interrogation of gene function without any pre-existing knowledge are needed to hasten understanding of parasite biology, which will expedite the identification of drug targets and the development of future interventions in the face of spreading resistance to existing frontline drugs. In this work, we describe a new approach to pursue forward-genetic phenotypic screens for P.?falciparum to identify factors associated with virulence. Future large-scale phenotypic screens developed to probe other such interesting phenomena, when considered in parallel, will prove a powerful tool for functional annotation of the P.?falciparum genome, where so much remains undiscovered.
机译:疟疾仍然是全球范围内最具破坏力的寄生虫病之一,2013年非洲90%的疟疾死亡归因于恶性疟原虫。疟疾的临床症状包括发烧,每48?h对应于红细胞的寄生虫破裂。与寄生虫能否抵抗宿主发烧反应的能力有关的寄生虫途径,实际上,约40%的恶性疟原虫基因的功能总体上仍然未知。在这里,我们评估了可扩展的前向遗传筛选方法的潜力,以鉴定参与宿主发烧反应的基因。我们利用先前研究中通过随机piggyBac转座子诱变产生的单干扰P.?falciparum突变体的选择,对与高热温度的寄生虫反应相关的基因进行了表型筛选。我们确定了几个突变体,与野生型相比,在高热反应筛查中表现出显着的表型,这表明了破坏基因在这一过程中的可能作用。我们提出这些初步研究,以证明正向遗传学可用于深入了解与寄生虫生物学相关的关键因素。重要性尽管恶性疟原虫的基因组序列已有多年历史,但其约40%的基因没有信息性注释,因为它们与被研究的生物没有可检测的同源性。还没有通过遗传方法评估更多。需要可扩展的前遗传方法,允许在没有任何现有知识的情况下询问基因功能,以加深对寄生虫生物学的了解,这将加速药物靶标的识别和面对现有一线药物耐药性扩散的未来干预措施的发展。在这项工作中,我们描述了一种新方法,可进行恶性疟原虫的前向表型筛选,以鉴定与毒力相关的因素。并行考虑,为探究其他此类有趣现象而开发的未来大规模表型筛选将证明是一种功能强大的工具,可用于恶性疟原虫基因组的功能注释,而目前仍有许多未被发现。

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