首页> 外文期刊>Biochemical Pharmacology >Rapid hydrolysis and slow alpha,beta-dicarbonyl cleavage of an agent proposed to cleave glucose-derived protein cross-links.
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Rapid hydrolysis and slow alpha,beta-dicarbonyl cleavage of an agent proposed to cleave glucose-derived protein cross-links.

机译:快速水解和慢速α,β-二羰基裂解剂可裂解葡萄糖衍生的蛋白质交联剂。

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摘要

The putative protein glycation cross-link cleaving agent N-phenacylthiazolium bromide (PTB) underwent hydrolysis and cyclic hemithioacetal formation under physiological conditions to form two isomeric 2,3-dihydro-4-formyl-2-hydroxy-2-phenyl-1,4-thiazines: at pH 7.4 and 37 degrees, the rate constant k(Hydrolysis) was (2.6+/-0.1) x 10(-4) sec and the chemical half-life was ca. 44 min. The alpha,beta-dicarbonyl cleavage reaction only competed effectively with the hydrolysis when the alpha,beta-dicarbonyl substrate was at nonphysiological high levels. The high concentrations of PTB (10-30 mM) used previously to demonstrate chemical and biochemical activity also lead to acidification of incubation media. The mechanism of action of PTB now requires reappraisal.
机译:在生理条件下,将假定的蛋白质糖基化交联裂解剂N-吩噻唑溴化铵(PTB)水解并形成环半硫缩醛,形成两个异构体2,3-二氢-4-甲酰基-2-羟基-2-苯基-1,4 -噻嗪:在pH 7.4和37度下,速率常数k(水解)为(2.6 +/- 0.1)x 10(-4)sec,化学半衰期为。 44分钟当α,β-二羰基底物处于非生理性高水平时,α,β-二羰基裂解反应仅与水解有效竞争。先前用于证明化学和生物化学活性的高浓度PTB(10-30 mM)也导致孵育培养基酸化。 PTB的行动机制现在需要重新评估。

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