Comparative pharmacodynamic analysis of imidazoline compounds using rat model of ocular mydriasis with a test of quantitative structure-activity relationships

Joanna Raczak-Gutknecht; Antoni Nasal; Teresa Frąckowiak; Anita Kornicka; Franciszek Sączewski; Renata Wawrzyniak; Łukasz Kubik; Roman Kaliszan

doi:10.1016/j.jpba.2017.03.053

Comparative pharmacodynamic analysis of imidazoline compounds using rat model of ocular mydriasis with a test of quantitative structure-activity relationships

J Pharm Biomed Anal. 2017 Sep 10:144:122-128. doi: 10.1016/j.jpba.2017.03.053. Epub 2017 Apr 6.

Authors

Joanna Raczak-Gutknecht¹, Antoni Nasal¹, Teresa Frąckowiak¹, Anita Kornicka², Franciszek Sączewski², Renata Wawrzyniak¹, Łukasz Kubik¹, Roman Kaliszan³

Affiliations

¹ Department of Biopharmaceutics and Pharmacodynamics, Medical University of Gdańsk, Gen. J. Hallera 107, 80-416 Gdańsk, Poland.
² Department of Chemical Technology of Drugs, Medical University of Gdańsk, Gen. J. Hallera 107, 80-416 Gdańsk, Poland.
³ Department of Biopharmaceutics and Pharmacodynamics, Medical University of Gdańsk, Gen. J. Hallera 107, 80-416 Gdańsk, Poland. Electronic address: roman.kaliszan@gumed.edu.pl.

PMID: 28420580
DOI: 10.1016/j.jpba.2017.03.053

Abstract

Imidazol(in)e derivatives, having the chemical structure similar to clonidine, exert diverse pharmacological activities connected with their interactions with alpha2-adrenergic receptors, e.g. hypotension, bradycardia, sedation as well as antinociceptive, anxiolytic, antiarrhythmic, muscle relaxant and mydriatic effects. The mechanism of pupillary dilation observed after systemic administration of imidazol(in)es to rats, mice and cats depends on the stimulation of postsynaptic alpha2-adrenoceptors within the brain. It was proved that the central nervous system (CNS)-localized I1-imidazoline receptors are not engaged in those effects. It appeared interesting to analyze the CNS-mediated pharmacodynamics of imidazole(in)e agents in terms of their chromatographic and calculation chemistry-derived parameters. In the present study a systematic determination and comparative pharmacometric analysis of mydriatic effects in rats were performed on a series of 20 imidazol(in)e agents, composed of the well-known drugs and of the substances used in experimental pharmacology. The eye pupil dilatory activities of the compounds were assessed in anesthetized Wistar rats according to the established Koss method. Among twenty imidazol(in)e derivatives studied, 18 produced diverse dose-dependent mydriatic effects. In the quantitative structure-activity relationships (QSAR) analysis, the pharmacological data (half maximum mydriatic effect - ED₅₀ in μmol/kg) were considered along with the structural parameters of the agents from molecular modeling. The theoretically calculated lipophilicity parameters, CLOGP, of imidazol(in)es, as well as their lipophilicity parameters from HPLC, logk_w, were also considered. The attempts to derive statistically significant QSAR equations for a full series of the agents under study were unsuccessful. However, for a subgroup of eight apparently structurally related imidazol(in)es a significant relationship between log(1/ED₅₀) and logk_w values was obtained. The lack of "predictive" QSAR for the whole series of the structurally diverse agents is probably due to a complex mechanism of the ligand-alpha2-adrenergic receptor interactions, which are predominantly of a highly structurally specific polar nature. Such interactions are difficult to quantify with the established chemical structural descriptors, contrary to the less specific, molecular bulkiness-related interactions.

Keywords: Imidazoline agents; Pharmacodynamic analysis; Quantitative structure–activity relationships (QSAR); Rat eye mydriasis; Structural descriptors.

MeSH terms

Animals
Cats
Imidazolines
Mice
Mydriasis*
Quantitative Structure-Activity Relationship
Rats
Rats, Wistar

Substances

Imidazolines