A comprehensive review on the pancreatic lipase inhibitory peptides: A future anti-obesity strategy

IF 1 Q3 MEDICINE, GENERAL & INTERNAL
Y. Tan, C. Gan, Muhammad Hakimin Shafie, P. Yap, A. Mohd Rodhi, Ashfaq Ahmad, V. Murugaiyah, M. Abdulla, E. Johns
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引用次数: 1

Abstract

Dysregulation of lipid homeostasis contributes to obesity and can directly lead to several critical public health concerns globally. This paper aimed to present a brief review of related properties and the use of pancreatic lipase inhibitors as the future weight loss drug discovery and development procured from a wide range of natural sources. A total of 176 pancreatic lipase inhibitory peptides were identified from recent publications and peptide databases. These peptides were classified into three categories according to their peptide length and further analyzed using bioinformatic approaches to identify their structural activity relationship. Molecular docking analyses were conducted for each amino acid at the terminal position of the peptides to predict the binding affinity between peptide-enzyme protein complexes based on intermolecular contact interactions. Overall, the observations revealed the features of the inhibitory peptides and their inhibitory mechanisms and interactions. These findings strived to benefit scientists whose research may be relevant to anti-obesity drug development and/or discovery thereby support effective translation of preclinical research for humans’ health being.
胰脂肪酶抑制肽研究综述:未来的抗肥胖策略
脂质稳态失调导致肥胖,并可直接导致全球几个关键的公共卫生问题。本文旨在简要介绍胰脂肪酶抑制剂的相关性质和用途,作为未来减肥药的发现和开发,从广泛的天然来源获得。从最近的出版物和肽数据库中共鉴定出176种胰脂肪酶抑制肽。根据这些肽的长度将其分为三类,并利用生物信息学方法进一步分析它们的结构活性关系。对肽末端的每个氨基酸进行分子对接分析,基于分子间接触相互作用预测肽-酶蛋白复合物之间的结合亲和力。总的来说,观察结果揭示了抑制肽的特征及其抑制机制和相互作用。这些发现努力使那些研究可能与抗肥胖药物开发和/或发现相关的科学家受益,从而支持有效地转化为人类健康的临床前研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Electronic Journal of General Medicine
Electronic Journal of General Medicine MEDICINE, GENERAL & INTERNAL-
CiteScore
3.60
自引率
4.80%
发文量
79
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