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Insight into GEBR-32a: Chiral Resolution Absolute Configuration and Enantiopreference in PDE4D Inhibition

机译:深入了解GEBR-32a:PDE4D抑制中的手性拆分绝对构型和对映体优先

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摘要

Alzheimer’s disease is the most common type of dementia, affecting millions of people worldwide. One of its main consequences is memory loss, which is related to downstream effectors of cyclic adenosine monophosphate (cAMP). A well-established strategy to avoid cAMP degradation is the inhibition of phosphodiesterase (PDE). In recent years, GEBR-32a has been shown to possess selective inhibitory properties against PDE type 4 family members, resulting in an improvement in spatial memory processes without the typical side effects that are usually correlated with this mechanism of action. In this work, we performed the HPLC chiral resolution and absolute configuration assignment of GEBR-32a. We developed an efficient analytical and semipreparative chromatographic method exploiting an amylose-based stationary phase, we studied the chiroptical properties of both enantiomers and we assigned their absolute configuration by H-NMR (nuclear magnetic resonance). Lastly, we measured the IC values of both enantiomers against both the PDE4D catalytic domain and the long PDE4D3 isoform. Results strongly support the notion that GEBR-32a inhibits the PDE4D enzyme by interacting with both the catalytic pocket and the regulatory domains.
机译:阿尔茨海默氏病是最常见的痴呆类型,影响着全球数百万人。其主要后果之一是记忆力丧失,这与环磷酸腺苷(cAMP)的下游效应子有关。避免cAMP降解的公认策略是抑制磷酸二酯酶(PDE)。近年来,已显示GEBR-32a具有针对PDE 4型家族成员的选择性抑制特性,从而改善了空间记忆过程,而没有通常与此作用机制相关的典型副作用。在这项工作中,我们进行了GEBR-32a的HPLC手性拆分和绝对构型分配。我们开发了一种利用基于直链淀粉的固定相的高效分析和半制备色谱方法,我们研究了两种对映异构体的手性,并通过H-NMR(核磁共振)确定了它们的绝对构型。最后,我们针对PDE4D催化域和长PDE4D3同工型测量了两种对映异构体的IC值。结果强烈支持GEBR-32a通过与催化口袋和调节域相互作用而抑制PDE4D酶的观点。

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