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Vol. 68 No. 7: Issue 7

Copyright (c) 2022 Munazzah Tasleem, Ambreen Shoaib, Asma Al-Shammary, Abdelmuhsin Abdelgadir, Zeina Alsamar, Qazi Mohammad Sajid Jamal, Abdulwahed Alrehaily, Fevzi Bardcki, Abdel Moneim E. Sulieman, Tarun Kumar Upadhyay, Irfan Ahmad Ansari, Dakun Lai, Riadh Badroui, Dharmendra Kumar Yadav, Mohd Saeed

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Computational analysis of PTP-1B site-directed mutations and their structural binding to potential inhibitors

Analysis of PTP-1B site-directed mutations
https://doi.org/10.14715/cmb/2022.68.7.13
Munazzah Tasleem
University of Electronic Science and Technology of China, Chengdu 610054, Sichuan, China
Ambreen Shoaib
Department of Pharmacy Practice, College of Pharmacy, Jazan University, P. Box No. 114, Jazan, Saudi Arabia
Asma Al-Shammary
Department of Public Health, College of Public Health and Health Informatics, University of Ha’il, P.O. Box 2240, Ha’il 81451, Saudi Arabia
Abdelmuhsin Abdelgadir
Department of Biology, College of Sciences, University of Hail, PO Box 2240, Hail, KSA
Zeina Alsamar
Department of Biology, College of Sciences, University of Hail, PO Box 2240, Hail, KSA
Qazi Mohammad Sajid Jamal
Department of Health Informatics, College of Public Health and Health Informatics, Qassim University, Al Bukayriyah, Saudi Arabia
Abdulwahed Alrehaily
Department of Biology, Faculty of Science, Islamic University of Madinah, P.O. Box 170, Madinah 42351, Saudi Arabia
Fevzi Bardcki
Department of Biology, College of Sciences, University of Hail, PO Box 2240, Hail, KSA
Abdel Moneim E. Sulieman
Department of Biology, College of Sciences, University of Hail, PO Box 2240, Hail, KSA
Tarun Kumar Upadhyay
Department of Biotechnology, Parul Institute of Applied Sciences and Animal Cell Culture and Immunobiochemistry Lab, Centre of Research for Development, Parul University, Vadodara 391760, India
Irfan Ahmad Ansari
Department of Biosciences, Integral University, Lucknow, India
Dakun Lai
School of Electronic Science and Engineering, University of Electronic Science and Technology of China, Chengdu 610054, Sichuan, China
Riadh Badroui
Department of Biology, College of Sciences, University of Hail, PO Box 2240, Hail, KSA
Dharmendra Kumar Yadav
College of Pharmacy, Gachon University of Medicine and Science, Yeonsu-gu, Incheon City, 21924, Korea
Mohd Saeed
Department of Biology, College of Sciences, University of Hail, PO Box 2240, Hail, KSA

Corresponding Author(s) : Mohd Saeed

mo.saeed@uoh.edu.sa

Cellular and Molecular Biology, Vol. 68 No. 7: Issue 7

Abstract

Protein tyrosine phosphatase-1B (PTP-1B) is a well-known therapeutic target for diabetes and obesity as it suppresses insulin and leptin signaling. PTP-1B deletion or pharmacological suppression boosted glucose homeostasis and insulin signaling without altering hepatic fat storage. Inhibitors of PTP-1B may be useful in the treatment of type 2 diabetes, and shikonin, a naturally occurring naphthoquinone dye pigment, is reported to inhibit PTP-1B and possess antidiabetic properties. Since the cell contains a large number of phosphatases, PTP-1B inhibitors must be effective and selective. To explore more about the mechanism underlying the inhibitor's efficacy and selectivity, we investigated its top four pharmacophores and used site-directed mutagenesis to insert amino acid mutations into PTP-1B as an extension of our previous study where we identified 4 pharmacophores of shikonin. The study aimed to examine the site-directed mutations like R24Y, S215E, and S216C influence the binding of shikonin pharmacophores, which act as selective inhibitors of PTP-1B. To achieve this purpose, docking and molecular dynamics simulations of wild-type (WT) and mutant PTP-1B with antidiabetic compounds were undertaken. The simulation results revealed that site-directed mutations can change the hydrogen bond and hydrophobic interactions between shikonin pharmacophores and many residues in PTP-1B's active site, influencing the drug's binding affinity. These findings could aid researchers in better understanding PTP-1B inhibitors' selective binding mechanism and pave the path for the creation of effective PTP-1B inhibitors.

Keywords

Multiple sequence alignment; phylogenetic tree; docking; intra-molecular interactions; site-directed mutagenesis; stability, MD simulation.
Tasleem, M. ., Shoaib, A. ., Al-Shammary, A. ., Abdelgadir, A. ., Alsamar, Z., Jamal, Q. M. S. ., Alrehaily, A. ., Bardcki, F. ., Sulieman, A. M. E. ., Upadhyay, T. K. ., Ansari, I. A., Lai, D. ., Badroui, R. ., Yadav, D. K. ., & Saeed, M. (2022). Computational analysis of PTP-1B site-directed mutations and their structural binding to potential inhibitors: Analysis of PTP-1B site-directed mutations. Cellular and Molecular Biology, 68(7), 75–84. https://doi.org/10.14715/cmb/2022.68.7.13
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