查尔酮
单胺氧化酶
单胺氧化酶B
塞莱吉林
单胺氧化酶A
化学
单胺类神经递质
对接(动物)
拉萨吉林
立体化学
药理学
生物化学
酶
医学
血清素
受体
帕金森病
内科学
护理部
疾病
作者
Athulya Krishna,Sunil Kumar,Sachithra Thazhathuveedu Sudevan,Ashutosh Kumar Singh,Leena K. Pappachen,T. M. Rangarajan,Mohamed A. Abdelgawad,Bijo Mathew,Bijo Mathew
出处
期刊:Cns & Neurological Disorders-drug Targets
[Bentham Science Publishers]
日期:2023-05-16
卷期号:23 (6): 697-714
被引量:6
标识
DOI:10.2174/1871527322666230515155000
摘要
Monoamine oxidase B is a crucial therapeutic target for neurodegenerative disorders like Alzheimer's and Parkinson's since they assist in disintegrating neurotransmitters such as dopamine in the brain. Pursuing efficacious monoamine oxidase B inhibitors is a hot topic, as contemporary therapeutic interventions have many shortcomings. Currently available FDA-approved monoamine oxidase inhibitors like safinamide, selegiline and rasagiline also have a variety of side effects like depression and insomnia. In the quest for a potent monoamine oxidase B inhibitor, sizeable, diverse chemical entities have been uncovered, including chalcones. Chalcone is a renowned structural framework that has been intensively explored for its monoamine oxidase B inhibitory activity.The structural resemblance of chalcone (1,3-diphenyl-2-propen-1-one) based compounds and 1,4-diphenyl- 2-butene, a recognized MAO-B inhibitor, accounts for their MAO-B inhibitory activity. Therefore, multiple revisions to the chalcone scaffold have been attempted by the researchers to scrutinize the implications of substitutions onthe molecule's potency. In this work, we outline the docking investigation results of various chalcone analogues with monoamine oxidase B available in the literature until now to understand the interaction modes and influence of substituents. Here we focused on the interactions between reported chalcone derivatives and the active site of monoamine oxidase B and the influence of substitutions on those interactions. Detailed images illustrating the interactions and impact of the substituents or structural modifications on these interactions were used to support the docking results.
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