The signaling nucleoside adenosine is produced intra- and extracellularly
under physiologic and, more importantly, under pathologic conditions. Adenosine
modulates cellular functions involved in injury, metabolic derangement, energy
perturbations, and inflammation. The biologic effects of adenosine are mediated by
four adenosine receptor (AR) subtypes of the G-protein coupled receptors (GPCRs)
family: A1AR, A2AAR, A2BAR and A3AR. In the cardiovascular (CV) system, adenosine
and its receptors are intricately involved in the regulation of myocardial contraction,
heart rate, sympathetic control, conductivity, vascular tone, cardiac and vascular
growth, inflammation, injury and apoptosis. As such, the modulation of the
adenosinergic system has therapeutic potential for cardiovascular diseases (CVDs) such
as metabolic disorders, atherosclerosis, hypertrophy, ischemic heart diseases, and heart
failure. Nevertheless, despite the many years of investigation and experimentation only
a few drugs targeting the adenosinergic system were developed and actually have
reached clinical application. This chapter outlines the unique role adenosine plays in
the CV system in physiology, pathology, and potentially therapeutic pharmacology. It
also presents an updated review of the different adenosine receptors ligands, and their
clinical potential in different CVDs.
Keywords: 4′-oxonucleosides, 4′-selenonucleoside, Adenosine, Adenosine
receptors, Allosteric modulator, Atherosclerosis, Binding affinity, Capadenoson,
Cardiac hypertrophy, Cardiovascular system, CGS 21680, Heart failure, Ischemic
heart disease, Istradefylline, Metabolic disorders, Receptor dimerization, Receptor
desensitization, Regadenoson, Rolofylline, Tecadenoson, Xanthine.
