Synthesis, Molecular Docking, Anti-cholinesterase Activity, Theoretical Investigation, and Catalytic Effect of New Encumbered N-benzyladamantyl Substituted Imidazolidin-2-ylidene Carbene Pd-PEPPSI Complexes

Author:

Ikhlef Sofiane12ORCID,Lasmari Sarra34ORCID,Zendaoui Saber Mustapha56ORCID,Mokrani El Hassen7ORCID,Tebbani Dahmane8,Gürbüz Nevin910,Bensouici Chawki11,Boulcina Raouf312,Zouchoune Bachir56,Özdemir Ismail910ORCID

Affiliation:

1. Laboratoire d’Obtention de Substances Thérapeutiques (LOST), Campus Caabet Ersas, Université Constantine 1, Constantine 25000, Algeria

2. Department of Technical Science, Institute of Sciences and Technology, Abd el Hafid Boussouf-Mila University Center, Mila 43000, Algeria

3. Laboratory of Synthesis of Molecules with Biological Interest, Faculty of Exact Sciences, Mentouri- Constantine 1 University, Constantine 25000, Algeria

4. Department of Biology, Faculty Natural and Life Sciences, Ferhat Abbas University-Setif 1, Setif 19000, Algeria

5. Laboratoire de Chimie Appliquée et Technologie des Matériaux, Université Larbi Ben M’Hidi Oum El Bouaghi, Oum El Bouaghi 04000, Algeria

6. Unité de Recherche de Chimie de l’Environnement et Moléculaire Structurale, Université Constantine (Mentouri), Constantine 25000, Algeria

7. Laboratory of Applied Biochemistry, Department of Biochemistry and Cellular and Molecular Biology, Faculty of Natural and Life Sciences, Mentouri-Constantine 1 University, Constantine 25000, Algeria

8. Laboratory of Natural Products of Plant Origin and Organic Synthesis, Department of Chemistry, Faculty of Exact Sciences, University of Constantine 1, Constantine 25000, Algeria

9. Catalysis Research and Application Center, Inönü University, Malatya 44280, Turkey

10. Department of Chemistry, Faculty of Science and Art, Inönü University, Malatya 44280, Turkey

11. Biotechnology Research Center, Constantine 25000, Algeria

12. Department of Engineering Process, Faculty of Technology, Mostefa Benboulaïd-Batna 2 University, Batna 5000, Algeria

Abstract

Abstract: This study aimed to describe the preparation of novel PEPPSI type Pd(II)-NHC complexes bearing N-benzyladamantyl substituted imidazolidin-2-ylidene group. All synthesized compounds were characterized by using 1H-NMR and 13C-NMR spectroscopies, FTIR, and elemental analysis techniques. One of the objectives of this study was the synthesis of Pd-NHC complexes with AChE/BChE inhibition activities. Among all the tested compounds, complexes 4b and 4c were found to have the most high potential AChE and BChE inhibitory activities with IC50 values of 21.57 ± 0.23 Mm and 15.78 ± 0.39 Mm, respectively. Conducting molecular docking studies helped us in gathering crucial information about the main binding interactions of inhibitors and enzymes, and the results were in agreement with the biological evaluation. The synthesized Pd-NHC complexes were employed for catalyzing the direct C2- and C5-arylation reaction between aryl (hetero) halide and a variety of heterocyclic systems. In both cases (C2 and C5-arylation), Pd-NHC complexes catalysts provided access to the arylated heterocycles in good to high yields in the presence of 1 mol% catalyst loading at 150°C. The DFT theoretical investigation showed that the Pd-NHC complexes were of ML2X2 type, where the the Pd(II) cation had a square planar geometry. The interaction energies obtained by energy decomposition analysis (EDA) demonstrated that the 4d and 4e complexes were more stable in the presence of more methyl substituents. The chemical indicators demonstrated that the less stable 4c complex was more reactive in regard to the chemical hardness, chemical potential, and electrophilicity values.

Funder

Technological and Scientific Research Council of Turkey TÜBİTAK

Publisher

Bentham Science Publishers Ltd.

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