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肉豆蔻与格列美脲联合用于2型糖尿病的一种可能替代疗法:体内评估与计算机模拟支持

A possible alternative therapy for type 2 diabetes using Myristica fragrans Houtt in combination with glimepiride: in vivo evaluation and in silico support.

作者信息

Nasreen Waheeda, Sarker Suchitra, Sufian Md Abu, Md Opo F A Dain, Shahriar Mohammad, Akhter Rumana, Halim Mohammad A

机构信息

Department of Pharmacy, School of Medicine, University of Asia Pacific, 74/A Green Road, Dhaka 1215, Bangladesh, Phone: +8801711737697.

Department of Pharmacy, School of Medicine, University of Asia Pacific, 74/A Green Road, Dhaka 1215, Bangladesh.

出版信息

Z Naturforsch C J Biosci. 2020 Mar 26;75(3-4):103-112. doi: 10.1515/znc-2019-0134.

DOI:10.1515/znc-2019-0134
PMID:32187019
Abstract

The current study aimed to evaluate the in vivo hypoglycemic potential of Myristica fragrans seed extract co-administered with glimepiride in Swiss albino mice. Computational tools were used to further verify the in vivo findings and to help compare this combination to the glimepiride-pioglitazone combination in terms of the binding affinity of the ligands to their respective target protein receptors and the relative stability of the drug-protein complexes. The effect of the combined therapy was observed both in alloxan- and glucose-induced hyperglycemic Swiss albino mice. The mean fasting blood glucose level of the test groups was measured and statistically evaluated using Student's t test. The combined therapy significantly reduced the blood glucose level in a time-dependent manner compared to glimepiride alone. The binding affinity of glimepiride was found to be -7.6 kcal/mol with sulfonylurea receptor 1 in molecular docking. Conversely, macelignan-peroxisome proliferator-activated receptor (PPAR) α and macelignan-PPAR γ complexes were stabilized with -9.2 and -8.3 kcal/mol, respectively. Molecular dynamic simulation revealed that macelignan-PPAR α and γ complexes were more stable than pioglitazone complexes. The combination shows promise in animal and computer models and requires further trials to provide evidence of its activity in humans.

摘要

本研究旨在评估肉豆蔻种子提取物与格列美脲联合给药对瑞士白化小鼠的体内降血糖潜力。使用计算工具进一步验证体内研究结果,并帮助将该组合与格列美脲-吡格列酮组合在配体与各自靶蛋白受体的结合亲和力以及药物-蛋白复合物的相对稳定性方面进行比较。在四氧嘧啶和葡萄糖诱导的高血糖瑞士白化小鼠中均观察到联合治疗的效果。测量测试组的平均空腹血糖水平,并使用学生t检验进行统计学评估。与单独使用格列美脲相比,联合治疗以时间依赖性方式显著降低血糖水平。在分子对接中,发现格列美脲与磺酰脲受体1的结合亲和力为-7.6千卡/摩尔。相反,肉豆蔻脂素-过氧化物酶体增殖物激活受体(PPAR)α和肉豆蔻脂素-PPARγ复合物分别以-9.2和-8.3千卡/摩尔的能量稳定。分子动力学模拟显示,肉豆蔻脂素-PPARα和γ复合物比吡格列酮复合物更稳定。该组合在动物和计算机模型中显示出前景,需要进一步试验以提供其在人类中的活性证据。

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