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Molecular cloning and characterization of a novel immunoreactive ATPase/RNA helicase in human filarial parasite Brugia malayi

机译:新型人丝虫寄生性马来虫中免疫反应性ATPase / RNA解旋酶的分子克隆与鉴定

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摘要

DEAD box proteins are putative RNA unwinding proteins found in organisms ranging from mammals to bacteria. We have identified a novel immunodominant cDNA clone, BmL3-helicase, encoding DEAD box RNA helicase by immunoscreening of a larval stage cDNA library of Brugia malayi. The cDNA sequence exhibited strong sequence homology to Caenorhabditis elegans and C. briggsae RNA helicase, a prototypic member of the DEAD (Asp-Glu-Ala-Asp) box protein family. The clone also showed similarity with RNA helicase of Wolbachia, an endosymbiotic bacterium of filarial parasite. It was overexpressed as ∼50 kDa His-tag fusion protein, and ATP hydrolysis assay of recombinant enzyme showed that either ATP or dATP was required for the unwinding activity, indicating BmL3-helicase as an ATP/dATP-dependent RNA helicase. The recombinant protein also demonstrated cross-seroreactivity with human bancroftian sera. The presence of BmL3-helicase in various life stages of B. malayi was confirmed by immunoblotting of parasite-life-cycle extracts with polyclonal sera against the BmL3-helicase, which showed high levels of expression in microfilaria, L3, and adult (both male and female) stages. In the absence of an effective macrofilaricidal agent and validated anti-filarial drug targets, RNA helicases could be utilized as a rational drug target for developing agents against the human filarial parasite.
机译:DEAD盒蛋白是从哺乳动物到细菌的生物体中发现的推定的RNA解链蛋白。我们已经确定了一种新的免疫优势的cDNA克隆,BmL3-解旋酶,通过对马来亚布鲁吉虫的幼虫期cDNA文库进行免疫筛选来编码DEAD框RNA解旋酶。该cDNA序列与秀丽隐杆线虫和Briggsae RNA解旋酶(DEAD(Asp-Glu-Ala-Asp)盒蛋白家族的原型成员)具有很强的序列同源性。该克隆还显示出与毛虫内生共生细菌Wolbachia的RNA解旋酶相似。它被过表达为约50 kDa的His-tag融合蛋白,重组酶的ATP水解分析表明,解旋活性需要ATP或dATP,这表明BmL3-解旋酶是依赖ATP / dATP的RNA解旋酶。重组蛋白还显示出与人班克罗夫特血清的交叉血清反应。通过用多克隆血清针对BmL3-解旋酶对寄生虫生命周期提取物进行免疫印迹,证实了马来芽孢杆菌各个生命阶段中BmL3-解旋酶的存在,后者在微丝aria,L 3,< / sub>和成人(男性和女性)阶段。在没有有效的大杀线虫剂和经过验证的抗孝性药物靶标的情况下,RNA解旋酶可以用作开发抗人丝虫原性药物的合理药物靶标。

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