调节过氧化物酶体增殖物激活受体-γ、环氧化酶-2和碳酸酐酶的多靶点格列酮用于代谢功能障碍的管理。

IF 4.9 Q1 CHEMISTRY, MEDICINAL

ACS Pharmacology and Translational Science Pub Date : 2025-05-23 eCollection Date: 2025-06-13 DOI:10.1021/acsptsci.5c00011

Perihan A Elzahhar, Hisham A Nematalla, Malak A Abouayana, El Sayed H El Ashry, Mahmoud Balbaa, Andrea Petreni, Rasha Nassra, Hend A Yassin, Yasmine N Kamel, Mohamed A Elrewiny, Mahmoud A Agami, Monica Makkar, Minh Sai, Daniel Merk, Hala F Labib, Rosaria Spagnuolo, Marina Naldi, Manuela Bartolini, Soad A El-Hawash, Claudiu T Supuran, Ahmed S F Belal, Ahmed F El-Yazbi

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引用次数: 0

摘要

鉴于在代谢疾病进展的不同阶段炎症改变与代谢功能障碍之间的显著相关性，我们专注于利用我们之前表征的格列酮衍生的抗炎1,2,3-三唑作为先导化合物，在代谢紊乱的框架内创建新的多靶点定向配体，与COX-2、过氧化物酶体增殖体激活受体γ (PPARγ)和CA相互作用。值得注意的是，有7种化合物表现出与塞来昔布相当或相似的COX-2抑制作用。4个化合物3b、3e、5e和5h对hCA I、II、IV和IX亚型（ki分别为8.5-833、0.37-24.6、44.2-777和27.3-32.1 nM）表现出明显的纳摩尔抑制作用。此外，化合物5e和5h在大鼠半膈实验中显示出显著增加葡萄糖摄取，优于吡格列酮。在荧光素酶测定中，PPARγ具有强大的激动作用，在不人为增加其表达的情况下，全长人PPARγ被激活，等温滴定量热法测定了kd，以证实它们的PPARγ依赖性胰岛素增敏活性。进行了体内药代动力学和组织分布实验，显示出良好的性能。在福尔马林诱导的大鼠足水肿实验中，其体外活性反映为有效的体内抗炎潜力，并且它们也表现出良好的溃疡形成特征。此外，对两个最活跃的分子5e和5h进行了计算靶点预测和网络药理学分析，确定了与预期结果相关的重要生物学途径。因此，5e和5h不仅可以减轻体内2型糖尿病大鼠模型的高血糖和胰岛素抵抗，还可以防止代谢功能障碍引起的肾脏和血脂损害。最后，对接模拟显示了与预期生物靶点的潜在结合相互作用。

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Multi-Target Glitazones for Modulating Peroxisome Proliferator-Activated Receptor-γ, Cyclooxygenase-2, and Carbonic Anhydrases for the Management of Metabolic Dysfunction.

In light of the significant correlation between inflammatory alterations and metabolic dysfunction throughout different stages of metabolic disease progression, we focused on utilizing our previously characterized glitazone-derived anti-inflammatory 1,2,3-triazoles as lead compounds to create new multitarget directed ligands that interact with COX-2, peroxisome proliferator-activated receptor γ (PPARγ), and CA within the framework of metabolic disorders. Notably, seven compounds exhibited equivalent or similar COX-2 inhibitory effects to celecoxib. Four compounds, namely, 3b, 3e, 5e, and 5h, exhibited substantial nanomolar inhibitory effects against hCA I, II, IV, and IX isoforms (K _i 8.5-833, 0.37-24.6, 44.2-777, and 27.3-32.1 nM, respectively). Furthermore, compounds 5e and 5h demonstrated a significant increase in glucose uptake in the rat hemidiaphragm experiment, outperforming pioglitazone. A robust PPARγ agonism in luciferase assay, full-length human PPARγ transactivation without artificially increasing its expression, and isothermal titration calorimetry for K _d determination were used to substantiate their PPARγ-dependent insulin-sensitizing activity. In vivo pharmacokinetic and tissue distribution experiments were carried out, revealing favorable properties. The in vitro activities were reflected into effective in vivo anti-inflammatory potential in the formalin-induced rat paw edema assay, and they also exhibited a favorable ulcerogenic profile. Furthermore, computational target prediction and network pharmacology analysis for the two most active molecules, 5e and 5h, identified important biological pathways associated with the intended outcomes. In this regard, 5e and 5h not only mitigated hyperglycemia and insulin resistance in an in vivo rat model of type 2 diabetes but also protected against renal and lipemic damage caused by metabolic dysfunction. Finally, docking simulations indicated potential binding interactions with the intended biological targets.

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来源期刊

ACS Pharmacology and Translational Science Medicine-Pharmacology (medical)

CiteScore

10.00

自引率

3.30%

发文量

133

期刊介绍： ACS Pharmacology & Translational Science publishes high quality, innovative, and impactful research across the broad spectrum of biological sciences, covering basic and molecular sciences through to translational preclinical studies. Clinical studies that address novel mechanisms of action, and methodological papers that provide innovation, and advance translation, will also be considered. We give priority to studies that fully integrate basic pharmacological and/or biochemical findings into physiological processes that have translational potential in a broad range of biomedical disciplines. Therefore, studies that employ a complementary blend of in vitro and in vivo systems are of particular interest to the journal. Nonetheless, all innovative and impactful research that has an articulated translational relevance will be considered. ACS Pharmacology & Translational Science does not publish research on biological extracts that have unknown concentration or unknown chemical composition. Authors are encouraged to use the pre-submission inquiry mechanism to ensure relevance and appropriateness of research.