Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Alexandria University, Alexandria, 21521, Egypt.
Department of Pharmacology and Therapeutics, Faculty of Pharmacy, Beirut Arab University, Tarik El Jadida, Riad El Solh, Beirut Campus, P.o box 11-5020, Beirut, 11072809, Lebanon.
Inflammopharmacology. 2024 Aug;32(4):2395-2411. doi: 10.1007/s10787-024-01501-3. Epub 2024 Jun 10.
Quinone-containing compounds have risen as promising anti-inflammatory targets; however, very little research has been directed to investigate their potentials. Accordingly, the current study aimed to design and synthesize group of quinones bearing different substituents to investigate the effect of these functionalities on the anti-inflammatory activities of this important scaffold. The choice of these substituents was carefully done, varying from a directly attached heterocyclic ring to different aromatic moieties linked through a nitrogen spacer. Both in vitro and in vivo anti-inflammatory activities of the synthesized compounds were assessed relative to the positive standards: celecoxib and indomethacin. The in vitro enzymatic and transcription inhibitory actions of all the synthesized compounds were tested against cyclooxygenase-2 (COX-2), cyclooxygenase-1 (COX-1), and 5-lipoxygenase (LOX) and the in vivo gene expression of Interleukin-1, interleukin 10, and Tumor Necrosis Factor-α (TNF-α) were determined. The IC against COX-1 and COX-2 enzymes obtained by the immunoassay test revealed promising activities of sixteen compounds with selectivity indices higher than 100-fold COX-2 selectivity. Out of those, four compounds revealed selectivity indices comparable to celecoxib as a reference drug. Furthermore, all the tested compounds inhibited LOX with an IC in the range of 1.59-3.11 µM superior to that of the reference drug used; zileuton (IC = 3.50 µM). Consequently, these results highlight the promising LOX inhibitory activity of the tested compounds. The obtained in vivo paw edema results showed high inhibitory percentage for the compounds 9a, 9b, and 11a with the significant lower TNF-α relative mRNA expression for compounds 5a, 5d, 9a, 9b, 12d, and 12e. Finally, in silico docking of the most active compounds (5b, 5d, 9a, 9b) against COX2 enzymes presented an acceptable justification of the obtained in vitro inhibitory activities. As a conclusion, Compounds 5b, 5d, 9a, 9b, and 11b showed promising results and thus deserves further investigation.
含醌类化合物已成为有前途的抗炎靶点;然而,针对它们的潜力进行研究的却很少。因此,本研究旨在设计和合成一组带有不同取代基的醌类化合物,以研究这些官能团对这一重要支架抗炎活性的影响。这些取代基的选择是经过精心挑选的,从直接连接的杂环到通过氮间隔基连接的不同芳基部分。与阳性标准:塞来昔布和吲哚美辛相比,评估了合成化合物的体外和体内抗炎活性。所有合成化合物的体外酶和转录抑制作用均针对环加氧酶-2(COX-2)、环加氧酶-1(COX-1)和 5-脂氧合酶(LOX)进行了测试,并测定了白细胞介素-1、白细胞介素 10 和肿瘤坏死因子-α(TNF-α)的体内基因表达。免疫测定试验获得的对 COX-1 和 COX-2 酶的 IC 揭示了 16 种化合物具有有希望的活性,其选择性指数高于 100 倍 COX-2 选择性。在这些化合物中,有 4 种化合物的选择性指数与塞来昔布作为参考药物相当。此外,所有测试的化合物均以优于参考药物齐留通(IC = 3.50 μM)的 IC 抑制 LOX,范围为 1.59-3.11 μM。因此,这些结果突出了测试化合物具有有希望的 LOX 抑制活性。获得的体内爪肿胀结果显示化合物 9a、9b 和 11a 的抑制百分比很高,化合物 5a、5d、9a、9b、12d 和 12e 的 TNF-α相对 mRNA 表达显著降低。最后,对最活跃的化合物(5b、5d、9a、9b)对 COX2 酶的计算机对接研究提供了对体外抑制活性的合理解释。总之,化合物 5b、5d、9a、9b 和 11b 表现出有希望的结果,因此值得进一步研究。
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