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对被忽视的动物寄生虫——微小泰勒虫的脱氧hypusine合酶进行靶向评估及其与疟原虫的关系。

Target evaluation of deoxyhypusine synthase from Theileria parva the neglected animal parasite and its relationship to Plasmodium.

作者信息

Njuguna James T, von Koschitzky Imke, Gerhardt Heike, Lämmerhofer Michael, Choucry Ali, Pink Mario, Schmitz-Spahnke Simone, Bakheit Mohammed A, Strube Christina, Kaiser Annette

机构信息

Institute for Pharmacogenetics, Medical Research Centre, University Duisburg-Essen, Germany.

Pharmaceutical Analytics, Pharmaceutical Institute, Eberhard-Karls-University Tübingen, Germany.

出版信息

Bioorg Med Chem. 2014 Aug 1;22(15):4338-46. doi: 10.1016/j.bmc.2014.05.007. Epub 2014 May 21.

Abstract

East Coast fever (ECF) is a tick-borne disease caused by the parasite Theileria parva which infects cattle. In Sub-Saharan Africa it leads to enormous economic costs. After a bite of a tick, sporozoites invade the host lymphocytes and develop into schizonts. At this stage the parasite transforms host lymphocytes resulting in the clonal expansion of infected lymphocytes. Animals develop a lymphoma like disorder after infection which is rapidly fatal. Hitherto, a few drugs of the quinone type can cure the disease. However, therapy can only be successful after early diagnosis. The genera Theileria and Plasmodium, which includes the causative agent of human malaria, are closely related apicomplexan parasites. Enzymes of the hypusine pathway, a posttranslational modification in eukaryotic initiation factor EIF-5A, have shown to be druggable targets in Plasmodium. We identified the first enzyme of the hypusine pathway from T. parva, the deoxyhypusine synthase (DHS), which is located on chromosome 2 of the Muguga strain. Transcription is significantly increased in schizonts. The expressed T. parva DHS reveals an open reading frame (ORF) of 370 amino acids after expression in Escherichia coli Rosetta cells with a molecular size of 41.26 kDa and a theoretical pI of 5.26. Screening of the Malaria Box which consists of 400 active compounds resulted in a novel heterocyclic compound with a guanyl spacer which reduced the activity of T. parva DHS to 45%. In sum, the guanyl residue seems to be an important lead structure for inhibition of Theileria DHS. Currently, more different guanyl analogues from the Malaria Box are tested in inhibitor experiments to determine their efficacy.

摘要

东海岸热(ECF)是一种由感染牛的寄生虫小泰累尔梨形虫引起的蜱传疾病。在撒哈拉以南非洲,它会导致巨大的经济损失。蜱叮咬后,子孢子侵入宿主淋巴细胞并发育成裂殖体。在此阶段,寄生虫会转化宿主淋巴细胞,导致受感染淋巴细胞的克隆扩增。动物感染后会发展成类似淋巴瘤的疾病,且迅速致命。迄今为止,少数醌类药物可以治愈这种疾病。然而,治疗只有在早期诊断后才能成功。泰勒虫属和疟原虫属(包括人类疟疾的病原体)是密切相关的顶复门寄生虫。在真核起始因子EIF - 5A的翻译后修饰——hypusine途径中的酶,已被证明是疟原虫的可药物作用靶点。我们从小泰累尔梨形虫中鉴定出了hypusine途径的第一种酶——脱氧hypusine合酶(DHS),它位于穆古加菌株的2号染色体上。在裂殖体中,转录显著增加。在大肠杆菌Rosetta细胞中表达后,表达的小泰累尔梨形虫DHS显示出一个370个氨基酸的开放阅读框(ORF),分子大小为41.26 kDa,理论pI为5.26。对由400种活性化合物组成的疟疾盒进行筛选,得到了一种带有胍基间隔基的新型杂环化合物,它将小泰累尔梨形虫DHS的活性降低到了45%。总之,胍基残基似乎是抑制泰勒虫DHS的重要先导结构。目前,正在抑制剂实验中测试更多来自疟疾盒的不同胍基类似物,以确定它们的疗效。

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