Computational and ADMET Predictions of Novel Compounds as Dual Inhibitors of BuChE and GSK-3β to Combat Alzheimer’s Disease

Saurabh G. Londhe; Vinayak Walhekar; Mangala Shenoy; Suvarna G. Kini; Marcus T. Scotti; Luciana Scotti; Dileep Kumar

doi:10.3390/pharmaceutics16080991

Pharmaceutics (Jul 2024)

Computational and ADMET Predictions of Novel Compounds as Dual Inhibitors of BuChE and GSK-3β to Combat Alzheimer’s Disease

Saurabh G. Londhe,
Vinayak Walhekar,
Mangala Shenoy,
Suvarna G. Kini,
Marcus T. Scotti,
Luciana Scotti,
Dileep Kumar

Affiliations

Saurabh G. Londhe: Department of Pharmaceutical Chemistry, BVDU’s Poona College of Pharmacy, Pune 411038, India
Vinayak Walhekar: Department of Pharmaceutical Chemistry, BVDU’s Poona College of Pharmacy, Pune 411038, India
Mangala Shenoy: Department of Pharmaceutical Chemistry, Manipal College of Pharmaceutical Sciences, Manipal Academy of Higher Education, Manipal 576104, India
Suvarna G. Kini: Department of Pharmaceutical Chemistry, Manipal College of Pharmaceutical Sciences, Manipal Academy of Higher Education, Manipal 576104, India
Marcus T. Scotti: Health Sci. Center, Federal University of Paraíba, João Pessoa 50670-910, PB, Brazil
Luciana Scotti: Health Sci. Center, Federal University of Paraíba, João Pessoa 50670-910, PB, Brazil
Dileep Kumar: Department of Pharmaceutical Chemistry, BVDU’s Poona College of Pharmacy, Pune 411038, India

DOI: https://doi.org/10.3390/pharmaceutics16080991
Journal volume & issue: Vol. 16, no. 8
p. 991

Abstract

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Background: Alzheimer’s disease is a serious and widespread neurodegenerative illness in the modern healthcare scenario. GSK-3β and BuChE are prominent enzymatic targets associated with Alzheimer’s disease. Co-targeting GSK3β and BChE in Alzheimer’s disease helps to modify disease progression and enhance cognitive function by addressing both tau pathology and cholinergic deficits. However, the treatment arsenal for Alzheimer’s disease is extremely inadequate, with present medications displaying dismal success in treating this never-ending ailment. To create novel dual inhibitors, we have used molecular docking and dynamics analysis. Our focus was on analogs formed from the fusion of tacrine and amantadine ureido, specifically tailored to target GSK-3β and BuChE. Methods: In the following study, molecular docking was executed by employing AutoDock Vina and molecular dynamics and ADMET predictions were performed using the Desmond and Qikprop modules of Schrödinger. Results: Our findings unveiled that compounds DKS1 and DKS4 exhibited extraordinary molecular interactions within the active domains of GSK-3β and BuChE, respectively. These compounds engaged in highly favorable interactions with critical amino acids, including Lys85, Val135, Asp133, and Asp200, and His438, Ser198, and Thr120, yielding encouraging docking energies of −9.6 and −12.3 kcal/mol. Additionally, through extensive molecular dynamics simulations spanning a 100 ns trajectory, we established the robust stability of ligands DKS1 and DKS4 within the active pockets of GSK-3β and AChE. Particularly noteworthy was DKS5, which exhibited an outstanding human oral absorption rate of 79.792%, transcending the absorption rates observed for other molecules in our study. Conclusion: In summary, our in silico findings have illuminated the potential of our meticulously designed molecules as groundbreaking agents in the fight against Alzheimer’s disease, capable of simultaneously inhibiting both GSK-3β and BuChE.

Published in Pharmaceutics

ISSN: 1999-4923 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceutics/

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