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Unraveling the importance of the malaria parasite helicases

机译:解开疟疾寄生虫螺旋酶的重要性

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Malaria is a human parasitic disease caused by infection from Plasmodium species, particularly Plasmodium falciparum. Each year millions of people are infected with malaria and large numbers of deaths result due to this deadly infection. P. falciparum contains 14 chromosomes, nearly 5400 genes and a multistage life cycle in humans and mosquitoes. The control of malaria is still a challenge as the parasite is continuously developing resistance to available antimalarial drugs and the mosquito vector is developing resistance to insecticides. The availability of P. falciparum genome has resulted in the identification of parasite-specific proteins that can be targeted without harmful effects to the human host. Toward this goal, we have been working on the identification and characterization of helicases in order to find parasite-specific helicases, which can be used as novel drug targets to tackle the rising problem of drug resistance. Helicases are ATP-dependent nucleic acid unwinding enzymes. The P. falciparum genome analysis depicts that it contains some parasite-specific helicases and homologs to most of the human helicases. Here, we present an overview of P. falciparum helicases and their importance in parasite growth and survival.
机译:疟疾是由来自疟原虫物种感染引起的人寄生疾病,特别是疟原虫疟原虫。由于这种致命的感染,每年有数百万人感染疟疾和大量死亡结果。 P. falciparum含有14个染色体,近5400个基因和人类和蚊子的多级生命周期。疟疾对疟疾的控制仍然是挑战,因为寄生虫不断地对可用的抗疟药药物耐药性,并且蚊子载体是对杀虫剂的抗性。 p. falciparum基因组的可用性导致寄生虫特异性蛋白质,其可针对人宿主而没有有害影响。为了实现这一目标,我们一直在研究螺旋酶的鉴定和表征,以便找到特定于寄生虫的螺旋酶,这可以用作新的药物靶标以解决耐药性的上升问题。螺旋酶是ATP依赖性核酸退滤酶。 P. falciparum基因组分析描述它含有一些寄生虫特异性螺旋酶和大多数人螺旋酶的同源物。在这里,我们概述了P. Falciparum Helicase及其在寄生虫生长和生存中的重要性。

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