首页> 美国卫生研究院文献>PLoS Neglected Tropical Diseases >The Heme Biosynthetic Pathway of the Obligate Wolbachia Endosymbiont of Brugia malayi as a Potential Anti-filarial Drug Target
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The Heme Biosynthetic Pathway of the Obligate Wolbachia Endosymbiont of Brugia malayi as a Potential Anti-filarial Drug Target

机译:马来布鲁氏虫专性Wolbachia内生菌的血红素生物合成途径作为潜在的抗丝虫药物靶标

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摘要

BackgroundFilarial parasites (e.g., Brugia malayi, Onchocerca volvulus, and Wuchereria bancrofti) are causative agents of lymphatic filariasis and onchocerciasis, which are among the most disabling of neglected tropical diseases. There is an urgent need to develop macro-filaricidal drugs, as current anti-filarial chemotherapy (e.g., diethylcarbamazine [DEC], ivermectin and albendazole) can interrupt transmission predominantly by killing microfilariae (mf) larvae, but is less effective on adult worms, which can live for decades in the human host. All medically relevant human filarial parasites appear to contain an obligate endosymbiotic bacterium, Wolbachia. This alpha-proteobacterial mutualist has been recognized as a potential target for filarial nematode life cycle intervention, as antibiotic treatments of filarial worms harboring Wolbachia result in the loss of worm fertility and viability upon antibiotic treatments both in vitro and in vivo. Human trials have confirmed this approach, although the length of treatments, high doses required and medical counter-indications for young children and pregnant women warrant the identification of additional anti-Wolbachia drugs.
机译:背景丝虫寄生虫(例如马来亚布鲁加(Brugia malayi),肠粘膜小盘菌(Onchocerca volvulus)和班氏无荚菌(Wuchereria bancrofti))是淋巴丝虫病和盘尾丝虫病的致病因子,它们是最容易被忽视的热带病之一。迫切需要开发大型杀线虫药物,因为目前的抗丝虫化学疗法(例如,二乙基卡巴嗪[DEC],伊维菌素和阿苯达唑)可以主要通过杀死微丝aria虫(mf)幼虫来中断传播,但对成虫的效果较差,可以在人类宿主中生存数十年。所有医学上相关的人类丝虫寄生虫似乎都含有专性的内共生细菌,Wolbachia。该α-蛋白细菌共生分子已被认为是丝虫线虫生命周期干预的潜在目标,因为对携带Wolbachia的丝虫进行抗生素治疗会导致在体外和体内进行抗生素治疗后,蠕虫的繁殖力和生存力丧失。人体试验已经证实了这种方法,尽管治疗时间长,所需的大剂量剂量以及针对年幼儿童和孕妇的医学禁忌症可以确定其他抗沃尔巴赫菌药物。

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