An in silico Evaluation of Anti-diabetic Potential of Vasicine, A Quinazoline Alkaloid of Justicia adhatoda Linnaeus

K.S. Ravali, G. Sarathchandra, S. Kumary, P.L. Sujatha, T.A. Kannan, M. Parthiban
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Abstract

Background: Diabetes mellitus, a chronic metabolic disease with multiple secondary effects, is on the rise. Treatment of type II diabetes mellitus with phytochemicals is gaining importance to avoid secondary complications used in the treatment. Justicia adhatoda is said to be an evergreen perennial shrub with a multitude of uses, especially as a stimulant of the respiratory tract. Methods: Vasicine, a major alkaloid extracted from the leaves of the adhatoda was used in the current study to identify its antidiabetic activity through the Computer Aided Drug Design technique. The molecular docking technique was performed between vasicine and five different receptors Protein Tyrosine Phosphate 1B (PTP 1B), Glucose Transporter (GLUT2), Glucagon Like Peptide 1 (GLP-1) and Peroxisome Proliferator Activated Receptors (PPAR Ɣ) which are usually targeted by anti-diabetic drugs. The Libdock score for the interaction between the receptors and vasicine is indicative of the antidiabetic activity of the vasicine in various pathways. Result: PTP 1B presented the highest LibDock score of 101.46 indicating the antidiabetic property of vasicine.
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林尼厄斯的一种喹唑啉类生物碱--Vasicine 的抗糖尿病潜力的硅学评估
背景:糖尿病是一种慢性代谢性疾病,具有多种继发性影响,发病率呈上升趋势。利用植物化学物质治疗 II 型糖尿病以避免治疗过程中出现继发性并发症的重要性日益凸显。据说 Justicia adhatoda 是一种多年生常绿灌木,具有多种用途,尤其是作为呼吸道的兴奋剂。方法:本研究使用了从阿达朵叶中提取的一种主要生物碱--瓦西碱,通过计算机辅助药物设计技术确定其抗糖尿病活性。研究人员采用分子对接技术,将血管宁与抗糖尿病药物通常针对的五种不同受体:酪氨酸磷酸蛋白 1B (PTP 1B)、葡萄糖转运体 (GLUT2)、胰高血糖素样肽 1 (GLP-1) 和过氧化物酶体增殖激活受体 (PPAR Ɣ)进行了对接。受体与血管紧张素之间相互作用的 Libdock 评分表明血管紧张素在各种途径中的抗糖尿病活性。结果显示PTP 1B 的 LibDock 得分最高,为 101.46 分,表明了血管宁的抗糖尿病特性。
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