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抗甲状腺药物的设计:在2.30 Å分辨率下乳过氧化物酶与2-巯基咪唑复合物的结合研究及结构测定。

Design of anti-thyroid drugs: Binding studies and structure determination of the complex of lactoperoxidase with 2-mercaptoimidazole at 2.30 Å resolution.

作者信息

Sirohi Harsh V, Singh Prashant K, Iqbal Naseer, Sharma Pradeep, Singh Amit K, Kaur Punit, Sharma Sujata, Singh Tej P

机构信息

Department of Biophysics, All India Institute of Medical Sciences, New Delhi.

出版信息

Proteins. 2017 Oct;85(10):1882-1890. doi: 10.1002/prot.25342. Epub 2017 Jul 21.

DOI:10.1002/prot.25342
PMID:28653416
Abstract

Lactoperoxidase (LPO) belongs to mammalian heme peroxidase superfamily, which also includes myeloperoxidase (MPO), eosinophil peroxidase (EPO), and thyroid peroxidase (TPO). LPO catalyzes the oxidation of a number of substrates including thiocyanate while TPO catalyzes the biosynthesis of thyroid hormones. LPO is also been shown to catalyze the biosynthesis of thyroid hormones indicating similar functional and structural properties. The binding studies showed that 2-mercaptoimidazole (MZY) bound to LPO with a dissociation constant of 0.63 µM. The inhibition studies showed that the value of IC was 17 µM. The crystal structure of the complex of LPO with MZY showed that MZY bound to LPO in the substrate-binding site on the distal heme side. MZY was oriented in the substrate-binding site in such a way that the sulfur atom is at a distance of 2.58 Å from the heme iron. Previously, a similar compound, 3-amino-1,2,4-triazole (amitrole) was also shown to bind to LPO in the substrate-binding site on the distal heme side. The amino nitrogen atom of amitrole occupied the same position as that of sulfur atom in the present structure indicating a similar mode of binding. Recently, the structure of the complex of LPO with a potent antithyroid drug, 1-methylimidazole-2-thiol (methimazole, MMZ) was also determined. It showed that MMZ bound to LPO in the substrate-binding site on the distal heme side with 2 orientations. The position of methyl group was same in the 2 orientations while the positions of sulfur atom differed indicating a higher preference for a methyl group.

摘要

乳过氧化物酶(LPO)属于哺乳动物血红素过氧化物酶超家族,该家族还包括髓过氧化物酶(MPO)、嗜酸性粒细胞过氧化物酶(EPO)和甲状腺过氧化物酶(TPO)。LPO催化包括硫氰酸盐在内的多种底物的氧化,而TPO催化甲状腺激素的生物合成。LPO也已被证明能催化甲状腺激素的生物合成,这表明它们具有相似的功能和结构特性。结合研究表明,2-巯基咪唑(MZY)以0.63μM的解离常数与LPO结合。抑制研究表明,IC值为17μM。LPO与MZY复合物的晶体结构表明,MZY在远端血红素侧的底物结合位点与LPO结合。MZY在底物结合位点的取向使得硫原子与血红素铁的距离为2.58Å。此前,一种类似的化合物3-氨基-1,2,4-三唑(杀草强)也被证明在远端血红素侧的底物结合位点与LPO结合。杀草强的氨基氮原子在本结构中占据了与硫原子相同的位置,表明结合模式相似。最近,还确定了LPO与一种强效抗甲状腺药物1-甲基咪唑-2-硫醇(甲巯咪唑,MMZ)复合物的结构。结果表明,MMZ在远端血红素侧的底物结合位点以两种取向与LPO结合。两种取向中甲基的位置相同,而硫原子的位置不同,这表明对甲基有更高的偏好。

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