Distortion effect on the ligation of imidazoles to water-insoluble iron(III) porphyrin

Abstract

Axial ligands control the various chemical reactions triggered by heme proteins. Thus, studies on the reaction of iron porphyrin with ligands are important for understanding their functions. Here, a spectroscopic investigation was performed to clarify the distortion effect of the porphyrin ring on the ligation of imidazoles (imidazole (Im), 1-methyl- and 2-methylimidazole (1-MeIm and 2-MeIm)) to iron(III) porphyrin. The overall stability constant ([Formula: see text] was found to have increased, while [Formula: see text] decreased with increasing distortion of the porphyrin core. However, the [Formula: see text] of the tetraphenyl-substituted complex, which is considered the least distorted, was not minimal, while the [Formula: see text] was not maximal. These results suggest that the stability of bis-ligand iron(III) porphyrin complexes depends on the increase in the saddle-type distortion of the porphyrin, the type of distortion, and the steric hindrance at the surrounding substituents. Furthermore, the ligation of 1-MeIm to iron(III) porphyrin hydroxo complexes with the porphyrin ring distortion was investigated. The ligation of 1-MeIm to the iron(III) dodecaphenylporphyrin hydroxo complex (DPPFeOH) suggests that a reaction mechanism different from the general reaction mechanism may occur simultaneously, i.e., a simultaneous reaction. In addition, the [Formula: see text] of DPPFeOH was found to be approximately 15 times smaller than that of the chloride complex. The relationship between the distortion and stability of bis-ligands iron(III) porphyrin complexes obtained in this study is expected to assist in the elucidation of the model reaction of heme proteins.