Structure-Based Optimization and Biological Evaluation of Pancreatic Lipase Inhibitors as Novel Potential Antiobesity Agents

Kun Wei; Gang-Qiang Wang; Xue Bai; Yan-Fen Niu; He-Ping Chen; Chun-Nan Wen; Zheng-Hui Li; Ze-Jun Dong; Zhi-Li Zuo; Wen-Yong Xiong; Ji-Kai Liu

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Structure-Based Optimization and Biological Evaluation of Pancreatic Lipase Inhibitors as Novel Potential Antiobesity Agents

机译：基于结构的优化和胰腺脂肪酶抑制剂作为新型潜在的减肥药的生物学评价。

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The unusual fused β-lactone vibralactone was isolated from cultures of the basidiomycete Boreostereum vibrans and has been shown to significantly inhibit pancreatic lipase. In this study, a structure-based lead optimization of vibralactone resulted in three series of 104 analogs, among which compound C1 exhibited the most potent inhibition of pancreatic lipase, with an IC50 value of 14?nM. This activity is more than 3000-fold higher than that of vibralactone. The effect of compound C1 on obesity was investigated using high-fat diet (HFD)-induced C57BL/6?J obese mice. Treatment with compound C1 at a dose of 100?mg/kg significantly decreased HFD-induced obesity, primarily through the improvement of metabolic parameters, such as triglyceride levels.

机译：异常融合的β-内酯vibralactone是从担子菌Boreostereum vibrans的培养物中分离得到的，并已显示出可显着抑制胰腺脂肪酶。在这项研究中，对草酸内酯进行了基于结构的先导优化，得到了三个系列的104个类似物，其中化合物C1表现出对胰腺脂肪酶的最强抑制作用，IC50值为14？nM。该活性比维拉内酯高3000倍以上。使用高脂饮食（HFD）诱导的C57BL / 6？J肥胖小鼠研究了化合物C1对肥胖的影响。化合物C1的剂量为100？mg / kg的治疗，可显着降低HFD诱导的肥胖症，这主要是通过改善代谢参数（例如甘油三酸酯水平）来实现的。

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《Natural Products and Bioprospecting》 |2015年第3期|共29页
作者
Kun Wei; Gang-Qiang Wang; Xue Bai; Yan-Fen Niu; He-Ping Chen; Chun-Nan Wen; Zheng-Hui Li; Ze-Jun Dong; Zhi-Li Zuo; Wen-Yong Xiong; Ji-Kai Liu;
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中图分类生物化学;
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2. Structure-Based Lead Optimization and Biological Evaluation of BAX Direct Activators as Novel Potential Anticancer Agents [J] . Stornaiuolo Mariano, La Regina Giuseppe, Passacantilli Sara, Journal of Medicinal Chemistry . 2015,第5期

机译：作为新型潜在抗癌药的BAX直接激活剂的基于结构的先导优化和生物学评估
3. Structure-based design, synthesis and biological evaluation of a novel series of isoquinolone and pyrazolo[4,3-c]pyridine inhibitors of fascin 1 as potential anti-metastatic agents [J] . Francis Stuart, Croft Daniel, Schtittelkopf Alexander W., Bioorganic and Medicinal Chemistry Letters . 2019,第8期

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4. Identification of Novel Falcipain-2 Inhibitors as Potential Antimalarial Agents through Structure-Based Virtual Screening [C] . Honglin Li, Rolf Hilgenfeld, Hualiang Jiang, ICMSI;International conference of molecular simulations and applied informatics technologies . 2010

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5. Hit Identification for PKCzeta Inhibitors: Structure-Based Optimization, Virtual Screening, and Biological Evaluation. [D] . Wu, Xiaoxin. 2016

机译：PKCzeta抑制剂的命中鉴定：基于结构的优化，虚拟筛选和生物学评估。
6. Structure-Based Optimization and Biological Evaluation of Pancreatic Lipase Inhibitors as Novel Potential Antiobesity Agents [O] . Kun Wei, Gang-Qiang Wang, Xue Bai, 2015

机译：基于结构的优化和胰腺脂肪酶抑制剂作为新型潜在的抗肥胖药的生物评价。
7. Structure-Based Optimization and Biological Evaluation of Pancreatic Lipase Inhibitors as Novel Potential Antiobesity Agents [O] . 2015

机译：基于结构的优化和胰腺脂肪酶抑制剂作为新型潜在的抗肥胖药的生物评价。

Structure-Based Optimization and Biological Evaluation of Pancreatic Lipase Inhibitors as Novel Potential Antiobesity Agents

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