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Crystal structure of the Anopheles gambiae 3-hydroxykynurenine transaminase

机译:冈比亚按蚊3-羟基犬尿氨酸转氨酶的晶体结构

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摘要

In Anopheles gambiae, the vector for the most deadly malaria parasite Plasmodium falciparum, xanthurenic acid (XA) plays a key role in parasite gametogenesis and fertility. In mosquitoes, XA is produced by transamination of 3-hydroxykynurenine (3-HK), a reaction that represents the main route to prevent the accumulation of the potentially toxic 3-HK excess. Interfering with XA metabolism in A. gambiae therefore appears an attractive avenue for the development of malaria transmission-blocking drugs and insecticides. We have determined the crystal structure of A. gambiae 3-HK transaminase in its pyridoxal 5′-phosphate form and in complex with a newly synthesized competitive enzyme inhibitor. Structural inspection of the enzyme active site reveals the key molecular determinants for ligand recognition and catalysis. Major contributions toward inhibitor binding are provided by a salt bridge between the inhibitor carboxylate and Arg-356 and by a remarkable hydrogen bond network involving the anthranilic moiety of the inhibitor and backbone atoms of residues Gly-25 and Asn-44. This study may be useful for the structure-based design of specific enzyme inhibitors of potential interest as antimalarial agents.
机译:在冈比亚按蚊中,最致命的疟原虫恶性疟原虫,黄腐酸(XA)的载体在寄生虫的配子发生和繁殖中起关键作用。在蚊子中,XA是通过3-羟基犬尿氨酸(3-HK)的氨基转移产生的,该反应代表了防止潜在的有毒3-HK过量积累的主要途径。因此,干扰冈比亚曲霉XA代谢似乎是开发阻断疟疾传播的药物和杀虫剂的诱人途径。我们已经确定了吡喃醛5'-磷酸形式并与新合成的竞争性酶抑制剂复合的冈比亚土壤杆菌3-HK转氨酶的晶体结构。酶活性位点的结构检查揭示了配体识别和催化的关键分子决定因素。抑制剂羧酸盐和Arg-356之间的盐桥以及涉及抑制剂的邻氨基苯甲酸部分和残基Gly-25和Asn-44的骨架原子的显着氢键网络对抑制剂的结合起了主要作用。该研究对于作为抗疟药的潜在酶抑制剂的基于结构的设计可能有用。

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