Unusual binding mode of the 2S4R stereoisomer of the potent aldose reductase cyclic imide inhibitor fidarestat (2S4S) in the 15 K crystal structure of the ternary complex refined at 0.78 angstrom resolution: Implications for the inhibition mechanism

Zhao HT; Hazemann I; Mitschler A; Carbone V; Joachimiak A; Ginell S; Podjarny A; El-Kabbani O

首页> 外文期刊>Journal of Medicinal Chemistry >Unusual binding mode of the 2S4R stereoisomer of the potent aldose reductase cyclic imide inhibitor fidarestat (2S4S) in the 15 K crystal structure of the ternary complex refined at 0.78 angstrom resolution: Implications for the inhibition mechanism

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Unusual binding mode of the 2S4R stereoisomer of the potent aldose reductase cyclic imide inhibitor fidarestat (2S4S) in the 15 K crystal structure of the ternary complex refined at 0.78 angstrom resolution: Implications for the inhibition mechanism

机译：强醛糖还原酶环状酰亚胺抑制剂非达司他（2S4S）的2S4R立体异构体在以0.78埃精制的三元复合物的15 K晶体结构中的异常结合模式：对抑制机理的暗示

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The structure of human aldose reductase in complex with the 2S4R stereoisomer of the potent inhibitor Fidarestat ((2S,4S)-6-fluoro-2',5'-dioxospiro-[chroman-4,4'-imidazoline]-2-carboxamide) was determined at 15 K and a resolution of 0.78 angstrom. The structure of the complex provides experimental evidence for the inhibition mechanism in which Fidarestat is initially bound neutral and then becomes negatively charged by donating the proton at the 1'-position nitrogen of the cyclic imide ring to the N epsilon 2 atom of the catalytic His 110.

机译：与有效抑制剂Fidarestat（（2S，4S）-6-fluoro-2'，5'-dioxospiro- [chroman-4,4'-咪唑啉] -2-羧酰胺的2S4R立体异构体复合的人醛糖还原酶的结构）是在15 K和0.78埃的分辨率下确定的。配合物的结构为抑制机制提供了实验证据，在该机制中，Fidarestat最初与中性结合，然后通过将环状酰亚胺环1'-位氮上的质子提供给催化His的N epsilon 2原子而带负电荷。 110。

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《Journal of Medicinal Chemistry》 |2008年第5期|共4页
作者
Zhao HT; Hazemann I; Mitschler A; Carbone V; Joachimiak A; Ginell S; Podjarny A; El-Kabbani O;
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正文语种 eng
中图分类药学;
关键词
DIABETIC COMPLICATIONS; ULTRAHIGH-RESOLUTION; POLYOL PATHWAY; NITRIC-OXIDE; DRUG DESIGN; CONGENERS; ACID; ISOQUINOLINE-1; 3-DIONES; SPIROSUCCINIMIDE; DEHYDROGENASE;

机译：糖尿病并发症;超高分辨率;多元醇途径;一氧化氮;药物设计;药物;酸;异喹啉-1;3-二酮;螺糖亚胺;脱氢酶;

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1. Unusual binding mode of the 2S4R stereoisomer of the potent aldose reductase cyclic imide inhibitor fidarestat (2S4S) in the 15 K crystal structure of the ternary complex refined at 0.78 angstrom resolution: Implications for the inhibition mechanism [J] . Zhao HT, Hazemann I, Mitschler A, Journal of Medicinal Chemistry . 2008,第5期

机译：强醛糖还原酶环状酰亚胺抑制剂非达司他（2S4S）的2S4R立体异构体在以0.78埃精制的三元复合物的15 K晶体结构中的异常结合模式：对抑制机理的暗示
2. Ultrahigh resolution drug design. II. Atomic resolution structures of human aldose reductase holoenzyme complexed with Fidarestat and Minalrestat: implications for the binding of cyclic imide inhibitors. [J] . El Kabbani O, Darmanin C, Schneider TR, Proteins: Structure, Function, and Genetics . 2004,第4期

机译：超高分辨率药物设计。二。与Fidarestat和Minalrestat复合的人醛糖还原酶全酶的原子分辨结构：对环酰亚胺抑制剂结合的影响。
3. X-ray structure of the V301L aldo-keto reductase 1B10 complexed with NADP+ and the potent aldose reductase inhibitor fidarestat: Implications for inhibitor binding and selectivity [J] . RuizF.X., Cousido-SiahA., MitschlerA., Chemico-biological interactions . 2013,第1a3期

机译：V301L醛酮还原酶1B10与NADP +和有效的醛糖还原酶抑制剂非达司他复合的X射线结构：抑制剂结合和选择性的意义
4. Refined 1.8 A structure of human aldose reductase complexed with the potent inhibitor zopolrestat. [O] . D K Wilson, I Tarle, J M Petrash, 1993

机译：精制1.8与有效抑制剂zopolrestat复合的人醛糖还原酶的结构。
5. Refined 1.8 A structure of human aldose reductase complexed with the potent inhibitor zopolrestat. [O] . Wilson, D K, Tarle, I, Petrash, J M, 1993

机译：精制1.8与有效抑制剂zopolrestat复合的人醛糖还原酶的结构。

Unusual binding mode of the 2S4R stereoisomer of the potent aldose reductase cyclic imide inhibitor fidarestat (2S4S) in the 15 K crystal structure of the ternary complex refined at 0.78 angstrom resolution: Implications for the inhibition mechanism

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