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新型含 1,2,3-三唑片段的熊果酸衍生物:设计、合成及体内外抗炎活性。

New ursolic acid derivatives bearing 1,2,3-triazole moieties: design, synthesis and anti-inflammatory activity in vitro and in vivo.

机构信息

Jilin Medical University, Jilin, 132013, Jilin Province, People's Republic of China.

The Third People's Hospital of Dalian, Dalian, 116000, People's Republic of China.

出版信息

Mol Divers. 2022 Apr;26(2):1129-1139. doi: 10.1007/s11030-021-10236-0. Epub 2021 Jun 2.

Abstract

In order to discover novel anti-inflammatory agents, three series of compounds obtained by appending 1,2,3-triazole moieties on ursolic acid were designed and synthesized. All compounds have been screened for their anti-inflammatory activity by using an ear edema model. The potent anti-inflammatory compound was subjected to in vitro cyclooxygenase COX-1/COX-2 inhibition assays. In general, the derivatives were found to be potent anti-inflammatory activity. Especially, the compound 11b exhibited the strongest activity of all of the compounds prepared, with 82.81% inhibition after intraperitoneal administration, which was better than celecoxib as a positive control. Molecular docking results unclose the rationale for the interaction of the compound 11b with COX-2 enzyme. Further studies revealed that compound 11b exhibited effective COX-2 inhibitory activity, with half-maximal inhibitor concentration (IC) value of 1.16 µM and selectivity index (SI = 64.66) value close to that of celecoxib (IC = 0.93 µM, SI = 65.47). Taken together, these results could suggest a promising chemotype for development of new COX-2-targeting anti-inflammatory agent.

摘要

为了发现新型抗炎剂,设计并合成了将 1,2,3-三唑部分连接到熊果酸上得到的三个系列的化合物。所有化合物均通过耳肿胀模型筛选其抗炎活性。对具有强大抗炎活性的化合物进行体外环氧化酶 COX-1/COX-2 抑制测定。一般来说,发现这些衍生物具有很强的抗炎活性。特别是,化合物 11b 在所有制备的化合物中表现出最强的活性,腹腔给药后抑制率达到 82.81%,优于作为阳性对照的塞来昔布。分子对接结果揭示了化合物 11b 与 COX-2 酶相互作用的原理。进一步的研究表明,化合物 11b 表现出有效的 COX-2 抑制活性,半最大抑制浓度 (IC) 值为 1.16 μM,选择性指数 (SI) 值为 64.66,接近于塞来昔布 (IC = 0.93 μM,SI = 65.47)。总之,这些结果表明,该化合物可能是开发新型 COX-2 靶向抗炎药物的有前途的化学型。

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