Interaction of Iron(III)-5,10,15,20-Tetrakis (4-Sulfonatophenyl) Porphyrin with Chloroquine, Quinine and Quinidine

Autor:	Albert S. Lundemba, Zéphyrin G. Yav, Luc Van Meervelt, Colin C. Groom, Celine W. Kadima, Juliette Pradon, Matthieu Kokengo Bokolo, Pitchouna I. Kilunga, Pius T. Mpiana, Dikima D. Bibelayi, Philippe Vuka Tsalu
Jazyk:	angličtina
Rok vydání:	2017
Předmět:	Steric effects Aqueous solution Hydrogen bond Stereochemistry Materials Science (miscellaneous) Quinoline Binding constant Medicinal chemistry Porphyrin Industrial and Manufacturing Engineering chemistry.chemical_compound chemistry Ionic strength Business and International Management Quinuclidine
Popis:	Iron(III)-5,10,15,20-tetrakis(4-sulfonatophenyl) porphyrin (FeTPPS) is used as non-physiological metalloporphyrin model for the natural iron (III)-pro- toporphyrin IX (FePPIX) resulting from hemoglobin degradation to investi- gate ligand binding reactions in aqueous solution. Studies were conducted on the interaction of FeTPPS with Chloroquine, Quinine, and Quinidine, which are historically the most common quinoline-based drugs used to treat malaria, an infectious disease afflicting several hundred millions every year world- wide, mainly in tropical regions. Using UV-Visible spectrophotometry, the binding reaction was studied at pH 7.40 in purely aqueous solution, and in aqueous solution containing NaNO3 at concentration of 0.1 M. Fitted titration curves obtained were in agreement with experimental data according to a formation scheme of 1:1 complex (1 FeTPPS Î¼-oxo-dimer: 1 Antimalarial). Values of apparent binding constant (K) obtained were between 4.3 Ã 103 Mâ 1 to 7.59 Ã 104 Mâ 1, demonstrating that FeTPPS and the antimalarials formed stable complexes. The stability of the complex decreased when NaNO3 was added to the solution. This ionic strength dependence was ascribed to elec- trostatic effects. Quinine and Chloroquine interacted with FeTPPS stronger than Quinidine did. Chloroquine showed the strongest affinity to FeTPPS. These findings revealed the influence of steric and stereochemical factors. Molecular electrostatic potentials (MEP) calculated with Hartree-Fock theory argue in favor of Ï -Ï and electrostatic interactions between reaction partners as driving forces for the complex formation. In the case of FeTPPS: Chloro-quine interaction, it is suggested that an intramolecular hydrogen bond is formed between phenyl SOâ and quinuclidine N-H+ as additional force sta- bilizing the complex. Analysis of crystallographic data using the Cambridge Structural Database (CSD) gave evidence of the hydrogen bond formation between phenyl SOâ and N-H+ groups in 370 structures. ispartof: Crystal Structure Theory and Applications vol:6 pages:25-38 status: published
Databáze:	OpenAIRE
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