Safety issues of compounds acting on adenosinergic signalling.

J Pharm Pharmacol

Faculty of Medicine, University of Maribor, Maribor, Slovenia.

Published: July 2017

AI Article Synopsis

  • Research on adenosine and its receptors has focused on understanding their roles, but few drugs have been approved due to safety concerns, prompting an investigation into the toxicological effects of adenosinergic compounds.
  • Various compounds, including adenosine derivatives and non-nucleosides, often lack selectivity and can affect other signaling systems, leading to potential genotoxicity and adverse effects.
  • The review summarizes safety data for these compounds, highlights mechanisms of toxicity, and discusses specific organ-related toxic effects observed in laboratory models.

Article Abstract

Objectives: Much research has been performed on the field of identifying the roles of adenosine and adenosinergic signalling, but a relatively low number of marketing authorizations have been granted for adenosine receptor (AdR) ligands. In part, this could be related to their safety issues; therefore, our aim was to examine the toxicological and adverse effects data of different compounds acting on adenosinergic signalling, including different AdR ligands and compounds resembling the structure of adenosine. We also wanted to present recent pharmaceutical developments of experimental compounds that showed promising results in clinical trial setting.

Key Findings: Safety issues of compounds modulating adenosinergic signalling were investigated, and different mechanisms were presented. Structurally different classes of compounds act on AdRs, the most important being adenosine, adenosine derivatives and other non-nucleoside compounds. Many of them are either not selective enough or are targeting other targets of adenosinergic signalling such as metabolizing enzymes that regulate adenosine levels. Many other targets are also involved that are not part of adenosinergic signalling system such as GABA receptors, different channels, enzymes and others. Some synthetic AdR ligands even showed to be genotoxic.

Summary: Current review presents safety data of adenosine, adenosine derivatives and other non-nucleoside compounds that modulate adenosinergic signalling. We have presented different mechanisms that participate to an adverse effect or toxic outcome. A separate section also deals with possible organ-specific toxic effects on different in-vitro and in-vivo models.

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Source
http://dx.doi.org/10.1111/jphp.12720DOI Listing

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