Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors: CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis

Seema K. Bhagwat; Sachin V. Patil; Abraham Vidal-Limon; J. Oscar C. Jimenez-Halla; Balasaheb K. Ghotekar; Vivek D. Bobade; Irving David Pérez-Landa; Enrique Delgado-Alvarado; Fabiola Hernández-Rosas; Tushar Janardan Pawar

doi:10.3390/molecules30173651

Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors: CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis

Seema K. Bhagwat
, Sachin V. Patil
, Abraham Vidal-Limon
, J. Oscar C. Jimenez-Halla
, Balasaheb K. Ghotekar
, Vivek D. Bobade
, Irving David Pérez-Landa
, Enrique Delgado-Alvarado
, Fabiola Hernández-Rosas^*
, Tushar Janardan Pawar^*

^*Autore corrispondente per questo lavoro

Research Centre HPT Arts and RYK Science College (Affiliated to Savitribai Phule Pune University)
Instituto de Ecologia, A.C.
Universidad de Guanajuato
Tecnológico Nacional de México, Mexico City
Universidad Veracruzana
Universidad Autonoma Queretaro
Red de Estudios Moleculares Avanzados, Campus III, Instituto de Ecología A. C

Risultato della ricerca › peer review

3 Citazioni (Scopus)

Abstract

Type 2 diabetes mellitus (T2DM) remains a global health challenge, prompting the development of novel α-glucosidase inhibitors (AGIs) to regulate postprandial hyperglycemia. This study reports the design, synthesis, and evaluation of indole-based Schiff base derivatives (4a–j) bearing a fixed methoxy group at the C₅ position. This substitution was strategically introduced to enhance lipophilicity, electronic delocalization, and π-stacking within the enzyme active site. Among the series, compound 4g (3-bromophenyl) exhibited the highest inhibitory activity (IC₅₀ = 10.89 µM), outperforming the clinical reference acarbose (IC₅₀ = 48.95 µM). The mechanism was supported by in silico analyses, such as the Density Functional Theory (DFT), molecular electrostatic potential (MEP) mapping, and molecular dynamics simulations, and CNN-based docking revealed that 4g engages in stable hydrogen bonding and π–π interactions with key residues (Asp327, Asp542, and Phe649), suggesting a potent and selective mode of inhibition. In silico ADMET predictions indicated favorable pharmacokinetic properties. Together, these results establish C₅–methoxy substitution as a viable strategy to enhance α-glucosidase inhibition in indole-based scaffolds.

Lingua originale	English
Numero di articolo	3651
Rivista	Molecules
Volume	30
Numero di pubblicazione	17
DOI	https://doi.org/10.3390/molecules30173651
Stato di pubblicazione	Published - 8 set 2025

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10.3390/molecules30173651

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https://www.scopus.com/pages/publications/105015594274

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Bhagwat, S. K., Patil, S. V., Vidal-Limon, A., Jimenez-Halla, J. O. C., Ghotekar, B. K., Bobade, V. D., Pérez-Landa, I. D., Delgado-Alvarado, E., Hernández-Rosas, F., & Pawar, T. J. (2025). Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors: CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis. Molecules, 30(17), Articolo 3651. https://doi.org/10.3390/molecules30173651

@article{c37a048715bc4b10b788457be62925bf,

title = "Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors: CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis",

abstract = "Type 2 diabetes mellitus (T2DM) remains a global health challenge, prompting the development of novel α-glucosidase inhibitors (AGIs) to regulate postprandial hyperglycemia. This study reports the design, synthesis, and evaluation of indole-based Schiff base derivatives (4a–j) bearing a fixed methoxy group at the C5 position. This substitution was strategically introduced to enhance lipophilicity, electronic delocalization, and π-stacking within the enzyme active site. Among the series, compound 4g (3-bromophenyl) exhibited the highest inhibitory activity (IC50 = 10.89 µM), outperforming the clinical reference acarbose (IC50 = 48.95 µM). The mechanism was supported by in silico analyses, such as the Density Functional Theory (DFT), molecular electrostatic potential (MEP) mapping, and molecular dynamics simulations, and CNN-based docking revealed that 4g engages in stable hydrogen bonding and π–π interactions with key residues (Asp327, Asp542, and Phe649), suggesting a potent and selective mode of inhibition. In silico ADMET predictions indicated favorable pharmacokinetic properties. Together, these results establish C5–methoxy substitution as a viable strategy to enhance α-glucosidase inhibition in indole-based scaffolds.",

keywords = "ADMET profiling, CNN-based docking, Schiff base derivatives, indole, molecular dynamics, type 2 diabetes mellitus, α-glucosidase inhibition",

author = "Bhagwat, \{Seema K.\} and Patil, \{Sachin V.\} and Abraham Vidal-Limon and Jimenez-Halla, \{J. Oscar C.\} and Ghotekar, \{Balasaheb K.\} and Bobade, \{Vivek D.\} and P{\'e}rez-Landa, \{Irving David\} and Enrique Delgado-Alvarado and Fabiola Hern{\'a}ndez-Rosas and Pawar, \{Tushar Janardan\}",

note = "Publisher Copyright: {\textcopyright} 2025 by the authors.",

year = "2025",

month = sep,

day = "8",

doi = "10.3390/molecules30173651",

language = "Ingl{\'e}s",

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Bhagwat, SK, Patil, SV, Vidal-Limon, A, Jimenez-Halla, JOC, Ghotekar, BK, Bobade, VD, Pérez-Landa, ID, Delgado-Alvarado, E, Hernández-Rosas, F & Pawar, TJ 2025, 'Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors: CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis', Molecules, vol. 30, n. 17, 3651. https://doi.org/10.3390/molecules30173651

TY - JOUR

T1 - Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors

T2 - CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis

AU - Bhagwat, Seema K.

AU - Patil, Sachin V.

AU - Vidal-Limon, Abraham

AU - Jimenez-Halla, J. Oscar C.

AU - Ghotekar, Balasaheb K.

AU - Bobade, Vivek D.

AU - Pérez-Landa, Irving David

AU - Delgado-Alvarado, Enrique

AU - Hernández-Rosas, Fabiola

AU - Pawar, Tushar Janardan

PY - 2025/9/8

Y1 - 2025/9/8

N2 - Type 2 diabetes mellitus (T2DM) remains a global health challenge, prompting the development of novel α-glucosidase inhibitors (AGIs) to regulate postprandial hyperglycemia. This study reports the design, synthesis, and evaluation of indole-based Schiff base derivatives (4a–j) bearing a fixed methoxy group at the C5 position. This substitution was strategically introduced to enhance lipophilicity, electronic delocalization, and π-stacking within the enzyme active site. Among the series, compound 4g (3-bromophenyl) exhibited the highest inhibitory activity (IC50 = 10.89 µM), outperforming the clinical reference acarbose (IC50 = 48.95 µM). The mechanism was supported by in silico analyses, such as the Density Functional Theory (DFT), molecular electrostatic potential (MEP) mapping, and molecular dynamics simulations, and CNN-based docking revealed that 4g engages in stable hydrogen bonding and π–π interactions with key residues (Asp327, Asp542, and Phe649), suggesting a potent and selective mode of inhibition. In silico ADMET predictions indicated favorable pharmacokinetic properties. Together, these results establish C5–methoxy substitution as a viable strategy to enhance α-glucosidase inhibition in indole-based scaffolds.

AB - Type 2 diabetes mellitus (T2DM) remains a global health challenge, prompting the development of novel α-glucosidase inhibitors (AGIs) to regulate postprandial hyperglycemia. This study reports the design, synthesis, and evaluation of indole-based Schiff base derivatives (4a–j) bearing a fixed methoxy group at the C5 position. This substitution was strategically introduced to enhance lipophilicity, electronic delocalization, and π-stacking within the enzyme active site. Among the series, compound 4g (3-bromophenyl) exhibited the highest inhibitory activity (IC50 = 10.89 µM), outperforming the clinical reference acarbose (IC50 = 48.95 µM). The mechanism was supported by in silico analyses, such as the Density Functional Theory (DFT), molecular electrostatic potential (MEP) mapping, and molecular dynamics simulations, and CNN-based docking revealed that 4g engages in stable hydrogen bonding and π–π interactions with key residues (Asp327, Asp542, and Phe649), suggesting a potent and selective mode of inhibition. In silico ADMET predictions indicated favorable pharmacokinetic properties. Together, these results establish C5–methoxy substitution as a viable strategy to enhance α-glucosidase inhibition in indole-based scaffolds.

KW - ADMET profiling

KW - CNN-based docking

KW - Schiff base derivatives

KW - indole

KW - molecular dynamics

KW - type 2 diabetes mellitus

KW - α-glucosidase inhibition

UR - https://www.scopus.com/pages/publications/105015594274

U2 - 10.3390/molecules30173651

DO - 10.3390/molecules30173651

M3 - Artículo

C2 - 40942175

AN - SCOPUS:105015594274

SN - 1420-3049

VL - 30

JO - Molecules

JF - Molecules

IS - 17

M1 - 3651

ER -

Design and Evaluation of Indole-Based Schiff Bases as α-Glucosidase Inhibitors: CNN-Enhanced Docking, MD Simulations, ADMET Profiling, and SAR Analysis

Abstract

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