| Literature DB >> 28488817 |
Daniel Meibom1, Barbara Albrecht-Küpper2, Nicole Diedrichs3, Walter Hübsch1, Raimund Kast2, Thomas Krämer1, Ursula Krenz1, Hans-Georg Lerchen1, Joachim Mittendorf1, Peter G Nell1, Frank Süssmeier1, Alexandros Vakalopoulos1, Katja Zimmermann4.
Abstract
Adenosine is known to be released under a variety of physiological and pathophysiological conditions to facilitate the protection and regeneration of injured ischemic tissues. The activation of myocardial adenosine A1 receptors (A1 Rs) has been shown to inhibit myocardial pathologies associated with ischemia and reperfusion injury, suggesting several options for new cardiovascular therapies. When full A1 R agonists are used, the desired protective and regenerative cardiovascular effects are usually overshadowed by unintended pharmacological effects such as induction of bradycardia, atrioventricular (AV) blocks, and sedation. These unwanted effects can be overcome by using partial A1 R agonists. Starting from previously reported capadenoson we evaluated options to tailor A1 R agonists to a specific partiality range, thereby optimizing the therapeutic window. This led to the identification of the potent and selective agonist neladenoson, which shows the desired partial response on the A1 R, resulting in cardioprotection without sedative effects or cardiac AV blocks. To circumvent solubility and formulation issues for neladenoson, a prodrug approach was pursued. The dipeptide ester neladenoson bialanate hydrochloride showed significantly improved solubility and exposure after oral administration. Neladenoson bialanate hydrochloride is currently being evaluated in clinical trials for the treatment of heart failure.Entities:
Keywords: adenosine A1 receptor; biological activity; dicyanopyridines; medicinal chemistry; partial agonists; prodrugs
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Year: 2017 PMID: 28488817 DOI: 10.1002/cmdc.201700151
Source DB: PubMed Journal: ChemMedChem ISSN: 1860-7179 Impact factor: 3.466