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Characterization of Two Distinct Structural Classes of Selective Aldehyde Dehydrogenase 1A1 Inhibitors

机译:选择性醛脱氢酶1A1抑制剂的两个不同结构类别的表征。

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摘要

Aldehyde dehydrogenases (ALDH) catalyze the irreversible oxidation of aldehydes to their corresponding carboxylic acid. Alterations in ALDH1A1 activity are associated with such diverse diseases as cancer, Parkinson’s disease, obesity, and cataracts. Inhibitors of ALDH1A1 could aid in illuminating the role of this enzyme in disease processes. However, there are no commercially available selective inhibitors for ALDH1A1. Here we characterize two distinct chemical classes of inhibitors that are selective for human ALDH1A1 compared to eight other ALDH isoenzymes. The prototypical members of each structural class, CM026 and CM037, exhibit sub-micromolar inhibition constants, but have different mechanisms of inhibition. The crystal structures of these compounds bound to ALDH1A1 demonstrate that they bind within the aldehyde binding pocket of ALDH1A1 and exploit the presence of a unique Glycine residue to achieve their selectivity. These two novel and selective ALDH1A1 inhibitors may serve as chemical tools to better understand the contributions of ALDH1A1 to normal biology and to disease states.
机译:醛脱氢酶(ALDH)催化醛不可逆地氧化为相应的羧酸。 ALDH1A1活性的改变与癌症,帕金森氏病,肥胖症和白内障等多种疾病有关。 ALDH1A1的抑制剂可以帮助阐明这种酶在疾病过程中的作用。但是,没有市售的ALDH1A1选择性抑制剂。在这里,我们描述了与其他八种ALDH同工酶相比对人ALDH1A1具有选择性的两种不同化学抑制剂。每种结构类别的原型成员CM026和CM037具有亚微摩尔抑制常数,但具有不同的抑制机制。这些与ALDH1A1结合的化合物的晶体结构表明它们结合在ALDH1A1的醛结合口袋中,并利用独特的甘氨酸残基的存在来实现其选择性。这两种新型的选择性ALDH1A1抑制剂可作为化学工具,以更好地了解ALDH1A1对正常生物学和疾病状态的贡献。

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  • 期刊名称 other
  • 作者单位
  • 年(卷),期 -1(58),4
  • 年度 -1
  • 页码 1964–1975
  • 总页数 30
  • 原文格式 PDF
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