Structure-activity and binding orientations analysis of potent, newly synthesized, acetylcholinesterase inhibitors

Krunić, Mihajlo; Penjišević, Jelena; Suručić, Relja; Šegan, Sandra; Kostić-Rajačić, Slađana; Jevtić, Ivana

doi:10.1016/j.molstruc.2022.134809

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2023

Authors

Krunić, Mihajlo

Penjišević, Jelena

Suručić, Relja

Šegan, Sandra

Kostić-Rajačić, Slađana
Jevtić, Ivana

Article (Published version)

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Abstract

Fourteen novel N-benzylpiperidine and N,N-diarylpiperazine conjugates were synthesized and pharmacologically evaluated as donepezil analogs, in a ligand-based drug design approach. All compounds possessed high to moderate in vitro inhibitory activity with IC50 in range 2.3–20 µM and selectivity towards acetylcholinesterase, while being inactive towards butyrylcholinesterase. Structure-activity relationship analysis revealed the influence of N,N-diarylpiperazine moiety and the linker connecting two pharmacophores on the inhibitory activity. Kinetic studies on the two most active compounds 7g and 8g (IC50 = 2.3 and 4 µM, respectively) revealed mixed type mode of inhibition, binding to both, free enzyme and enzyme-substrate complex. For further understanding of mechanism of action and binding orientations, molecular docking was performed for all compounds, while the ligand transport simulation and molecular dynamics simulations were performed for 7g and 8g. Computational results corrobora...

Keywords:

Alzheimer's disease / Arylpiperazine / Cholinesterase / Ligand transport simulation / Molecular docking / Molecular dynamics / N-benzylpiperidine

Source:
Journal of Molecular Structure, 2023, 1276, 134809-

Publisher:

Elsevier B.V.

Funding / projects:

Ministry of Education, Science and Technological Development, Republic of Serbia, Grant no. 200026 (University of Belgrade, Institute of Chemistry, Technology and Metallurgy - IChTM) (RS-200026)

DOI: 10.1016/j.molstruc.2022.134809

ISSN: 0022-2860; 1872-8014

WoS: 000904118100004

TY  - JOUR
AU  - Krunić, Mihajlo
AU  - Penjišević, Jelena
AU  - Suručić, Relja
AU  - Šegan, Sandra
AU  - Kostić-Rajačić, Slađana
AU  - Jevtić, Ivana
PY  - 2023
UR  - https://cer.ihtm.bg.ac.rs/handle/123456789/5634
AB  - Fourteen novel N-benzylpiperidine and N,N-diarylpiperazine conjugates were synthesized and pharmacologically evaluated as donepezil analogs, in a ligand-based drug design approach. All compounds possessed high to moderate in vitro inhibitory activity with IC50 in range 2.3–20 µM and selectivity towards acetylcholinesterase, while being inactive towards butyrylcholinesterase. Structure-activity relationship analysis revealed the influence of N,N-diarylpiperazine moiety and the linker connecting two pharmacophores on the inhibitory activity. Kinetic studies on the two most active compounds 7g and 8g (IC50 = 2.3 and 4 µM, respectively) revealed mixed type mode of inhibition, binding to both, free enzyme and enzyme-substrate complex. For further understanding of mechanism of action and binding orientations, molecular docking was performed for all compounds, while the ligand transport simulation and molecular dynamics simulations were performed for 7g and 8g. Computational results corroborated well with in vitro activities and kinetic studies.
PB  - Elsevier B.V.
T2  - Journal of Molecular Structure
T1  - Structure-activity and binding orientations analysis of potent, newly synthesized, acetylcholinesterase inhibitors
VL  - 1276
SP  - 134809
DO  - 10.1016/j.molstruc.2022.134809
ER  -

@article{
author = "Krunić, Mihajlo and Penjišević, Jelena and Suručić, Relja and Šegan, Sandra and Kostić-Rajačić, Slađana and Jevtić, Ivana",
year = "2023",
abstract = "Fourteen novel N-benzylpiperidine and N,N-diarylpiperazine conjugates were synthesized and pharmacologically evaluated as donepezil analogs, in a ligand-based drug design approach. All compounds possessed high to moderate in vitro inhibitory activity with IC50 in range 2.3–20 µM and selectivity towards acetylcholinesterase, while being inactive towards butyrylcholinesterase. Structure-activity relationship analysis revealed the influence of N,N-diarylpiperazine moiety and the linker connecting two pharmacophores on the inhibitory activity. Kinetic studies on the two most active compounds 7g and 8g (IC50 = 2.3 and 4 µM, respectively) revealed mixed type mode of inhibition, binding to both, free enzyme and enzyme-substrate complex. For further understanding of mechanism of action and binding orientations, molecular docking was performed for all compounds, while the ligand transport simulation and molecular dynamics simulations were performed for 7g and 8g. Computational results corroborated well with in vitro activities and kinetic studies.",
publisher = "Elsevier B.V.",
journal = "Journal of Molecular Structure",
title = "Structure-activity and binding orientations analysis of potent, newly synthesized, acetylcholinesterase inhibitors",
volume = "1276",
pages = "134809",
doi = "10.1016/j.molstruc.2022.134809"
}

Krunić, M., Penjišević, J., Suručić, R., Šegan, S., Kostić-Rajačić, S.,& Jevtić, I.. (2023). Structure-activity and binding orientations analysis of potent, newly synthesized, acetylcholinesterase inhibitors. in Journal of Molecular Structure
Elsevier B.V.., 1276, 134809.
https://doi.org/10.1016/j.molstruc.2022.134809

Krunić M, Penjišević J, Suručić R, Šegan S, Kostić-Rajačić S, Jevtić I. Structure-activity and binding orientations analysis of potent, newly synthesized, acetylcholinesterase inhibitors. in Journal of Molecular Structure. 2023;1276:134809.
doi:10.1016/j.molstruc.2022.134809 .

Krunić, Mihajlo, Penjišević, Jelena, Suručić, Relja, Šegan, Sandra, Kostić-Rajačić, Slađana, Jevtić, Ivana, "Structure-activity and binding orientations analysis of potent, newly synthesized, acetylcholinesterase inhibitors" in Journal of Molecular Structure, 1276 (2023):134809,
https://doi.org/10.1016/j.molstruc.2022.134809 . .