| Literature DB >> 33488253 |
Emre GÜzel1, Fatih SÖnmez2, Sultan Erkan3, Kübra ÇikrikÇi4, Adem ErgÜn4, Nahit GenÇer4, Oktay Arslan4, Makbule B KoÇak5.
Abstract
The investigation of carbonic anhydrase and paraoxonase enzyme inhibition properties of water-soluble zinc and gallium phthalocyanine complexes ( 1 and 2 ) are reported for the first time. The binding of p-sulfonylphenoxy moieties to the phthalocyanine structure favors excellent solubilities in water, as well as providing an inhibition effect on carbonic anhydrase (CA) I and II isoenzymes and paraoxonase (PON1) enzyme. According to biological activity results, both complexes inhibited hCA I, hCA II, and PON1. Whereas 1 and 2 showed moderate hCA I and hCA II (off-target cytosolic isoforms) inhibitory activity (Ki values of 26.09 µM and 43.11 µM for hCA I and 30.95 µM and 33.19 µM for hCA II, respectively), they exhibited strong PON1 (associated with high-density lipoprotein [HDL]) inhibitory activity (Ki values of 0.37 µM and 0.27 µM, respectively). The inhibition kinetics were analyzed by Lineweaver-Burk double reciprocal plots. It revealed that 1 and 2 were noncompetitive inhibitors against PON1, hCA I, and hCA II. These complexes can be more advantageous than other synthetic CA and PON inhibitors due to their water solubility. Docking studies were carried out to examine the interactions between hCA I, hCA II, and PON1 inhibitors and metal complexes at a molecular level and to predict binding energies.Entities:
Keywords: Phthalocyanine; carbonic anhydrase; enzyme inhibition; molecular docking; paraoxonase; sulfonated; water-soluble
Year: 2020 PMID: 33488253 PMCID: PMC7763127 DOI: 10.3906/kim-2007-21
Source DB: PubMed Journal: Turk J Chem ISSN: 1300-0527 Impact factor: 1.239