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首页> 外文期刊>The Journal of Experimental Biology >Recent advances in functional genomics for parasitic nematodes of mammals
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Recent advances in functional genomics for parasitic nematodes of mammals

机译:哺乳动物寄生线虫功能基因组学的最新进展

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摘要

Human-parasitic nematodes infect over a quarter of the world's population and are a major cause of morbidity in low-resource settings. Currently available treatments have not been sufficient to eliminate infections in endemic areas, and drug resistance is an increasing concern, making new treatment options a priority. The development of new treatments requires an improved understanding of the basic biology of these nematodes. Specifically, a better understanding of parasitic nematode development, reproduction and behavior may yield novel drug targets or new opportunities for intervention such as repellents or traps. Until recently, our ability to study parasitic nematode biology was limited because few tools were available for their genetic manipulation. This is now changing as a result of recent advances in the large-scale sequencing of nematode genomes and the development of new techniques for their genetic manipulation. Notably, skin-penetrating gastrointestinal nematodes in the genus Strongyloides are now amenable to transgenesis, RNAi and CRISPR/Cas9-mediated targeted mutagenesis, positioning the Strongyloides species as model parasitic nematode systems. A number of other mammalian-parasitic nematodes, including the giant roundworm Ascaris suum and the tissue-dwelling filarial nematode Brugia malayi, are also nowamenable to transgenesis and/or RNAi in some contexts. Using these tools, recent studies of Strongyloides species have already provided insight into the molecular pathways that control the developmental decision to form infective larvae and that drive the host-seeking behaviors of infective larvae. Ultimately, a mechanistic understanding of these processes could lead to the development of new avenues for nematode control.
机译:人寄生线虫在世界上四分之一的人口中感染,并且是低资源环境中发病率的主要原因。目前可用的治疗方法没有足以消除流行区域的感染,并且耐药性是越来越多的关注,使新的治疗方案成为优先事项。新治疗的发展需要改善对这些线虫的基本生物学的理解。具体而言,更好地了解寄生线虫发育,繁殖和行为可以产生新的药物目标或用于疏口或陷阱的干预的新机会。直到最近,我们研究寄生线虫生物学的能力是有限的,因为少量工具可用于其遗传操作。由于Nematode基因组的大规模排序和新技术的近期测序,这是由于近期进展而变化的。值得注意的是,酮酮的皮肤穿透性胃肠线虫现在适用于转基因,RNAi和CRASP / Cas9介导的靶向诱变,将抗酮化物种定位为模型寄生线虫系统。在一些其他哺乳动物 - 寄生线虫和包括巨蛔虫蛔虫和组织栖息的丝状线虫堡垒Malayi,在某些情况下也不是转基因和/或RNAi。使用这些工具,最近对抗酮物种的研究已经提供了对控制发育决定的分子途径的洞察力,并驱使感染幼虫的宿主寻找行为。最终,对这些流程的机制理解可能导致新途径的线虫控制。

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