High-resolution structures of Trypanosoma brucei pteridine reductase ligand complexes inform on the placement of new molecular entities in the active site of a potential drug target

机译：锥虫布鲁氏菌蝶啶还原酶配体复合物的高分辨率结构表明新分子实体在潜在药物靶标的活性位点中的位置

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Pteridine reductase (PTR1) is a potential target for drug development against parasitic Trypanosoma and Leishmania species. These protozoa cause serious diseases for which current therapies are inadequate. High-resolution structures have been determined, using data between 1.6 and 1.1 Å resolution, of T. brucei PTR1 in complex with pemetrexed, trimetrexate, cyromazine and a 2,4-diaminopyrimidine derivative. The structures provide insight into the interactions formed by new molecular entities in the enzyme active site with ligands that represent lead compounds for structure-based inhibitor development and to support early-stage drug discovery.

机译：蝶啶还原酶（PTR1）是针对寄生性锥虫和利什曼原虫物种的药物开发的潜在目标。这些原生动物引起严重的疾病，目前的治疗方法还不足以解决这些问题。使用1.6-1.1Å分辨率的布鲁氏菌PTR1与培美曲塞，曲美曲塞，环丙嗪和2,4-二氨基嘧啶衍生物的复合物，已确定了高分辨率的结构。这些结构提供了对酶活性位点中新分子实体与配体的相互作用的了解，这些配体代表用于基于结构的抑制剂开发并支持早期药物发现的先导化合物。

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期刊名称 Acta Crystallographica Section D: Biological Crystallography
作者
Alice Dawson; Lindsay B. Tulloch; Keri L. Barrack; William N. Hunter;
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年(卷),期 -1(66),0 12
年度 -1
页码 1334–1340
总页数 16
原文格式 PDF
正文语种
中图分类分子生物学;生化遗传学;生化药理学;生物物理学;
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外文文献

1. Structures of Leishmania major pteridine reductase complexes reveal the active site features important for ligand binding and to guide inhibitor design [J] . Schuttelkopf AW, Hardy LW, Beverley SM, Journal of Molecular Biology . 2005,第1期

机译：利什曼原虫主要蝶啶还原酶复合物的结构揭示了对配体结合和指导抑制剂设计重要的活性位点特征
2. Identification of Novel Potential Inhibitors of Pteridine Reductase 1 in Trypanosoma brucei via Computational Structure-Based Approaches and in Vitro Inhibition Assays [J] . Kimuda Magambo Phillip, Laming Dustin, Hoppe Heinrich C., Molecules . 2019,第1期

机译：通过基于计算结构的方法和体外抑制测定鉴定奈多肌瘤Brucei中蕨类植物还原酶1的新潜在抑制剂
3. Application of a simple quantum chemical approach to ligand fragment scoring for Trypanosoma brucei pteridine reductase 1 inhibition [J] . Jedwabny Wiktoria, Panecka-Hofman Joanna, Dyguda-Kazimierowicz Edyta, Journal of Computer-Aided Molecular Design . 2017,第8期

机译：一种简单的量子化学方法在锥虫瘤蕨类植物中的配体片段评分中的应用1抑制
4. In-Silico Studies of Essential Metabolic Reactions of Trypanosoma brucei: Identifying Potential Drug Targets [C] . Shalom Nwodo Chinedu, Segun A. Fatumo, Ezekiel F. Adebiyi International Conference on Bioinformatics, Computational Biology, Genomics and Chemoinformatics . 2010

机译：硅瘤瘤菌瘤菌瘤的基本代谢反应的硅研究：鉴定潜在的药物靶标
5. Evaluation of Trypanosoma brucei asparagine synthetase A and ribose 5-phosphate isomerase B as potential drug targets. [D] . Loureiro, Ines Marina Soares. 2015

机译：评价布鲁氏锥虫天冬酰胺合成酶A和核糖5磷酸异构酶B作为潜在的药物靶标。
6. Identification of Novel Potential Inhibitors of Pteridine Reductase 1 in Trypanosoma brucei via Computational Structure-Based Approaches and in Vitro Inhibition Assays [O] . Magambo Phillip Kimuda, Dustin Laming, Heinrich C. Hoppe, 2019

机译：通过基于计算结构的方法和体外抑制分析鉴定布鲁氏锥虫中新型Pteridine还原酶的潜在抑制剂
7. High-resolution structures of Trypanosoma brucei pteridine reductase ligand complexes inform on the placement of new molecular entities in the active site of a potential drug target [O] . Dawson, Alice, Tulloch, Lindsay B., Barrack, Keri L., 2010

机译：锥虫布鲁氏菌蝶啶还原酶配体复合物的高分辨率结构表明新分子实体在潜在药物靶标的活性位点中的位置

High-resolution structures of Trypanosoma brucei pteridine reductase ligand complexes inform on the placement of new molecular entities in the active site of a potential drug target

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