Coordination Chemistry of Cu 2+ Complexes of Small N-Alkylated Tetra-azacyclophanes with SOD Activity

Coordination Chemistry of Cu 2+ Complexes of Small N-Alkylated Tetra-azacyclophanes with SOD Activity

A new tetraaza-pyridinophane macrocycle (L1) N-alkylated with two isopropyl and one methyl groups symmetrically disposed has been prepared and its behavior compared with those of the unsubstituted pyridinophane (L3) and the related compound with three methyl groups (L2). The protonation studies show...

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Bibliographic Details
Published in:Inorganic chemistry Vol. 57; no. 17; pp. 10961 - 10973
Main Authors: Martínez-Camarena, Álvaro, Liberato, Andrea, Delgado-Pinar, Estefanía, Algarra, Andrés G, Pitarch-Jarque, Javier, Llinares, José M, Mañez, M Ángeles, Domenech-Carbó, Antonio, Basallote, Manuel G, García-España, Enrique
Format: Journal Article
Language:English
Published: United States 04-09-2018
Subjects:
Alkylating Agents - chemistry
Computer Simulation
Copper - chemistry
Hydrogen-Ion Concentration
Ions
Kinetics
Ligands
Molecular Conformation
Organometallic Compounds - chemistry
Organometallic Compounds - metabolism
Superoxide Dismutase - metabolism
X-Ray Diffraction
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Summary:A new tetraaza-pyridinophane macrocycle (L1) N-alkylated with two isopropyl and one methyl groups symmetrically disposed has been prepared and its behavior compared with those of the unsubstituted pyridinophane (L3) and the related compound with three methyl groups (L2). The protonation studies show that, first, a proton binds to the central methylated amine group of L1, while, second protonation leads to a reorganization of the protons that are at this stage attached to the lateral isopropylated amines. The X-ray structure of [HL1] agrees with the UV-vis and NMR studies as well as with the results of DFT calculations. The stability of the Cu complexes decreases on increasing the bulkiness of the alkyl substituents of the amine groups. The crystal structures of [CuL1Cl](ClO ) and [CuL1(H O)](ClO ) ·H O show square pyramidal coordination geometries with the ligands disposed in a bent L-shaped conformation. Kinetic studies indicate that the rates of both complexation and ligand dissociation decrease with the bulkiness of the substituents, so that the stability changes are surely the results of compensating effects, complex formation dominating over complex dissociation. The pH dependence of the rate constants for complex formation cannot be explained by consideration of rapid pre-equilibria involving the different protonated forms of the ligand, and it has been interpreted in terms of a mechanism involving an acid-base equilibrium for a reaction intermediate. NBT SOD studies show that the Cu complex of the bulkiest L1 ligand is the one having the highest activity (IC = 0.26(5) μM, k = 13.7 × 10 M s ) which can be associated with the poorer σ-donor ability of the tertiary amino groups, and the rigidity of the system, caused by the bulky isopropyl groups.
ISSN:0020-1669
1520-510X
DOI:10.1021/acs.inorgchem.8b01492