AI Article Synopsis
- Adenosine interacts with different receptors (A1, A2A, A3) in the heart, with significant focus on A2A due to its unclear role.
- Researchers created mice that overexpressed the A2A receptor, finding that this led to increased heart contractility and calcium handling, but effects diminished after 20 weeks.
- Overexpression of A2A enhanced survival and prevented heart failure in mice with high A1 receptor levels, indicating a crucial balance between A1 and A2A receptors for heart function and potential therapeutic implications.
Article Abstract
In the heart, adenosine binds to pharmacologically distinct G-protein-coupled receptors (A(1)-R, A(2A)-R, and A(3)-R). While the role of A(1)- and A(3)-Rs in the heart has been clarified, the effect of genetically manipulating the A(2A)-R has not been defined. Thus, we created mice overexpressing a cardiac-restricted A(2A)-R transgene. Mice with both low (Lo) and high (Hi) levels of A(2A)-R overexpression demonstrated an increase in cardiac contractility at 12 weeks. These changes were associated with a significantly higher systolic but not diastolic [Ca(2+)]i, higher maximal contraction amplitudes, and a significantly enhanced sarcoplasmic reticulum Ca(2+) uptake activity. At 20 weeks, the effects of A(2A)-R overexpression on cardiac contractility diminished. The positive effects elicited by A(2A)-R overexpression differ from the heart failure phenotype we observed with A(1)-R overexpression. Interestingly, coexpression of A(2A)-R TG(Hi), but not A(2A)-R TGLo, enhanced survival, prevented the development of left ventricular dysfunction and heart failure, and improved Ca(2+) handling in mice overexpressing the A(1)-R. These results suggest that adenosine-mediated signaling in the heart requires a balance between A(1)- and A(2A)-Rs--a finding that may have important implications for the ongoing clinical evaluation of adenosine receptor subtype-specific agonists and antagonists for the treatment of cardiovascular diseases.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2846643 | PMC |
| http://dx.doi.org/10.1111/j.1752-8062.2008.00027.x | DOI Listing |
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