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强效血管舒张剂的合成:6-(4-取代苯基)-3-哒嗪酮衍生物作为潜在肼屈嗪类似物的计算机模拟和体外评价。

Synthesis of potent vasodilating agents: in silico and in vitro evaluation of 6-(4-substitutedphenyl)-3-pyridazinone derivatives as potential hydralazine analogues.

机构信息

Pharmaceutical chemistry department, Faculty of Pharmacy, Misr International University, Cairo, Egypt.

Pharmaceutical organic chemistry department, Faculty of Pharmacy, Cairo University, Cairo, Egypt.

出版信息

Sci Rep. 2024 Nov 27;14(1):29514. doi: 10.1038/s41598-024-79697-1.

Abstract

People of all age categories and lifestyles suffer to different extents from hypertension. Accordingly, this necessitates the rise of new ways to defeat this enemy. Vasodilators exert a principal portion of highly effectual antihypertensive agents; our research is focused on the design, synthesis and biological evaluation of a new series of 6-(4-substitutedphenyl)-3-pyridazinones as potential hydralazine vasodilator analogues implementing both in vitro and in silico approaches. All the synthesized compounds were assessed for their vitro vasorelaxant activity against multiple references. New members revealed potent vasorelaxant activity (EC50 = 0.02916-1.907 µM) compared to the conventional vasorelaxants hydralazine, diazoxide, isosorbitole mononitrate and nitroglycerin (EC50 = 18.21, 19.5, 30.1 and 0.1824 µM, respectively). Compounds 2e, 2h and 2j exerted superior activities compared to others with EC50 = 0.1162, 0.07154 and 0.02916 µM, respectively. The physiochemical properties and drug-likeliness behavior of the new derivatives were investigated by conducting ADMET studies.

摘要

所有人都或多或少地受到高血压的困扰,不论年龄大小,生活方式如何。因此,需要寻找新的方法来对抗这一敌人。血管扩张剂在高效降压药物中起着主要作用;我们的研究集中在设计、合成和生物评估一系列新的 6-(4-取代苯基)-3-哒嗪酮作为潜在的肼屈嗪血管扩张剂类似物,同时采用体外和计算方法。所有合成的化合物都被评估了对多种参考物的体外血管舒张活性。与传统的血管舒张剂肼屈嗪、二氮嗪、异山梨醇单硝酸酯和硝化甘油(EC50=18.21、19.5、30.1 和 0.1824 μM 分别)相比,新成员表现出更强的血管舒张活性(EC50=0.02916-1.907 μM)。化合物 2e、2h 和 2j 的活性优于其他化合物,EC50 分别为 0.1162、0.07154 和 0.02916 μM。通过进行 ADMET 研究,研究了新衍生物的物理化学性质和药物相似性行为。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d6bd/11603188/4bac94ffc909/41598_2024_79697_Fig1_HTML.jpg

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