Electronegativity in Substituted-4(H)-quinazolinones Causes Anxiolysis without a Sedative-hypnotic Adverse Reaction in Female Wistar Rats.

Shweta Mishra, Debashree Das, Adarsh Sahu, Ekta Verma, Shailendra Patil, Ram Kishore Agarwal, Asmita Gajbhiye
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引用次数: 1

Abstract

Objective: In the current study, the synthesis, characterization, and neuropharmacology of quinazolinone tethered with aromatic (3a-3i) and heteroaromatic substitution (3j, 3k, and 3l) as effective anxiolytic agents are reported.

Background: Anxiety and depression are often comorbid with neurological as well as other medical maladies. Clinically known anxiolytics (Benzodiazepines) are accompanied by untoward sedation and other CNS depressive actions. The quinazolinone moiety is a privileged pharmacophore with a wide pharmacological spectrum. Herein, the synthesis, characterization, and neuropharmacological evaluation of some 2-substituted quinazolinone derivatives are reported.

Methods: The synthesized compounds were characterized using 1H-NMR and TLC analysis. Behavioral analysis was performed using EPM (Elevated Plus Maze), OFT (Open Field Test), PIST (Pentobarbital Induced Sleep Test), FST (Forced Swim Test) and PCPA (p-chlorophenyl alanine) bioassay. To further justify the therapeutic claim, systemic and neurotoxicological analysis of the most potent members of the series was performed using OECD mandated protocols. The studies showed that the compounds had a wide therapeutic window with >1000 mg/kg and >500 mg/kg LD50 and NOAEL, respectively.

Results: The compounds with an electronegative group in the quinazolinone nucleus (3f, 3e, 3d, and 3c) induced anxiolysis devoid of sedative adverse reaction. Besides, anti-depressant efficacy of 3f, 3e, 3d, and 3c observed in rodents was a result of a decrease in anxiety level. It was found that the neurotoxicology of the potent members (3f, 3e, 3d, and 3c) advocated their wide therapeutic window with >1000 mg/kg LD50 and >5000 mg/kg NOAEL.

Conclusion: Our findings of behavioral bioassays revealed that inducing an electronegative group into the quinazolinone nucleus yielded the most potent members of the series (3f, 3e, 3d, and 3c). The said compounds were found to produce anxiolysis and anti-depressive action without sedative-hypnotic side effects in rodent models. In summary, it can be stated that extending the studies in a clinical setting would furbish the contours of current anxiolytic therapy, especially in anxiety comorbid with medical maladies.

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取代-4(H)-喹唑啉酮的电负性引起雌性Wistar大鼠的抗焦虑性,无镇静催眠不良反应。
目的:本研究报道了芳香(3a-3i)和杂芳香取代(3j, 3k和3l)的喹唑啉酮的合成、表征和神经药理学。背景:焦虑和抑郁通常与神经系统疾病以及其他医学疾病共病。临床上已知的抗焦虑药(苯二氮卓类药物)伴有不良镇静和其他中枢神经系统抑郁行为。喹唑啉酮部分是一种具有广泛药理谱的特殊药效团。本文报道了一些2-取代喹唑啉酮衍生物的合成、表征和神经药理学评价。方法:采用1H-NMR和TLC对合成的化合物进行表征。行为学分析采用EPM (Elevated Plus Maze)、OFT (Open Field Test)、PIST(戊巴比妥诱导睡眠试验)、FST(强迫游泳试验)和PCPA(对氯苯丙氨酸)生物测定法。为了进一步证明治疗声称的合理性,使用经合组织授权的协议对该系列中最有效的成员进行了系统和神经毒理学分析。研究表明,该化合物的LD50和NOAEL分别>1000 mg/kg和>500 mg/kg,具有较宽的治疗窗口。结果:喹唑啉酮核中含有电负性基团(3f、3e、3d和3c)的化合物具有抗焦虑作用,无镇静不良反应。此外,3f、3e、3d和3c在啮齿动物体内的抗抑郁作用是由于焦虑水平的降低。结果表明,强效成员(3f、3e、3d和3c)的神经毒理学表现为LD50 >1000 mg/kg、NOAEL >5000 mg/kg的治疗窗宽。结论:我们的行为生物测定结果表明,在喹唑啉酮细胞核中诱导一个电负性基团产生了该系列中最有效的成员(3f, 3e, 3d和3c)。所述化合物在啮齿动物模型中发现具有抗焦虑和抗抑郁作用,无镇静催眠副作用。总之,可以这样说,在临床环境中扩展研究将刷新当前抗焦虑疗法的轮廓,特别是在焦虑与医学疾病共病方面。
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来源期刊
Central nervous system agents in medicinal chemistry
Central nervous system agents in medicinal chemistry Psychology-Neuropsychology and Physiological Psychology
CiteScore
2.10
自引率
0.00%
发文量
21
期刊介绍: Central Nervous System Agents in Medicinal Chemistry aims to cover all the latest and outstanding developments in medicinal chemistry and rational drug design for the discovery of new central nervous system agents. Containing a series of timely in-depth reviews written by leaders in the field covering a range of current topics, Central Nervous System Agents in Medicinal Chemistry is an essential journal for every medicinal chemist who wishes to be kept informed and up-to-date with the latest and most important developments in the field.
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