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单胺氧化酶同工酶通过混合双突变体循环按功能基团细分对神经递质的选择。

Neurotransmitter selection by monoamine oxidase isoforms, dissected in terms of functional groups by mixed double mutant cycles.

机构信息

Biomolecular Sciences Research Centre, Sheffield Hallam University, Howard Street, Sheffield, S1 1WB, UK.

出版信息

Org Biomol Chem. 2019 Oct 21;17(39):8871-8877. doi: 10.1039/c9ob01558b. Epub 2019 Sep 26.

Abstract

Double mutant cycles were constructed using neurotransmitters and synthetic substrates that measure their selective binding to one monoamine oxidase (MAO) enzyme isoform over another as a function of structural change. This work measures a reduction in selectivity for the MAOB isoform of 3 to 9.5 kJ mol upon the addition of hydroxy functional groups to a phenethylamine scaffold. Replacement of hydroxy functional groups on the phenethylamine scaffold by hydrophobic substituents measures an increase in selectivity for MAOB of -1.1 to -6.9 kJ mol. The strategies presented here can be applied to the development of competitive reversible inhibitors of MAO enzymes and other targets with structurally related isoforms.

摘要

双突变体环被构建使用神经递质和合成底物,这些神经递质和合成底物可以测量它们对一种单胺氧化酶(MAO)酶同型体的选择性结合,而不是另一种,这是作为结构变化的函数。这项工作测量了在苯乙胺支架上添加羟基官能团后,对 MAOB 同型体的选择性降低了 3 到 9.5 kJ/mol。在苯乙胺支架上用疏水性取代基取代羟基官能团,测量对 MAOB 的选择性增加了-1.1 到-6.9 kJ/mol。这里提出的策略可以应用于 MAO 酶和其他具有结构相关同型体的靶标的竞争性可逆抑制剂的开发。

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