The discovery of a selective and potent A2a agonist with extended lung retention

Annika B M Åstrand; Eva Lamm Bergström; Hui Zhang; Lena Börjesson; Therese Söderdahl; Cecilia Wingren; Anne-Helene Jansson; Amir Smailagic; Camilla Johansson; Håkan Bladh; Igor Shamovsky; Anders Tunek; Tomas Drmota

doi:10.1002/prp2.134

The discovery of a selective and potent A2a agonist with extended lung retention

Pharmacol Res Perspect. 2015 Jun;3(3):e00134. doi: 10.1002/prp2.134. Epub 2015 May 4.

Affiliations

¹ RIA iMed, AstraZeneca R&D Mölndal SE-431 59, Mölndal, Sweden.
² Drug Safety & Metabolism, AstraZeneca R&D Mölndal SE-431 59, Mölndal, Sweden.
³ AstraZeneca R&D Lund SE-221 87, Lund, Sweden.

Abstract

Although the anti-inflammatory role of the A2a receptor is well established, controversy remains with regard to the therapeutic value for A2a agonists in treatment of inflammatory lung diseases, also as a result of unwanted A2a-mediated cardiovascular effects. In this paper, we describe the discovery and characterization of a new, potent and selective A2a agonist (compound 2) with prolonged lung retention and limited systemic exposure following local administration. To support the lead optimization chemistry program with compound selection and profiling, multiple in vitro and in vivo assays were used, characterizing compound properties, pharmacodynamics (PD), and drug concentrations. Particularly, pharmacokinetic-PD modeling was applied to quantify the effects on the cardiovascular system, and an investigative toxicology study in rats was performed to explore potential myocardial toxicities. Compound 2, in comparison to a reference A2a agonist, UK-432,097, demonstrated higher solubility, lower lipophilicity, lower plasma protein binding, high rat lung retention (28% remaining after 24 h), and was efficacious in a lung inflammatory rat model following intratracheal dosing. Despite these properties, compound 2 did not provide a sufficient therapeutic index, that is, separation of local anti-inflammatory efficacy in the lung from systemic side effects in the cardiovascular system. The plasma concentration that resulted in induction of hypotension (half maximal effective concentration; EC50 0.5 nmol/L) correlated to the in vitro A2a potency (rIC50 0.6 nmol/L). Histopathological lesions in the heart were observed at a dose level which is threefold above the efficacious dose level in the inflammatory rat lung model. In conclusion, compound 2 is a highly potent and selective A2a agonist with significant lung retention after intratracheal administration. Despite its local anti-inflammatory efficacy in rat lung, small margins to the cardiovascular effects suggested limited therapeutic value of this compound for treatment of inflammatory lung disease by the inhaled route.

Keywords: A2a; Adenosine receptor; blood pressure; heart rate; inflammation; lung retention; pharmacokinetic-pharmacodynamic; therapeutic window.