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Adenosine regulation of the immune response initiated by ischemia reperfusion injury

Journal

PERFUSION-UK
Volume 31, Issue 2, Pages 103-110

Publisher

SAGE PUBLICATIONS LTD
DOI: 10.1177/0267659115586579

Keywords

reperfusion; cardioplegia; adenosine; lymphocyte; neutrophil; macrophage

Funding

  1. Steinbronn Heart Failure Research Award

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It is clinically established that adenosine has negative chronotropic, antiarrhythmic effects and reduces arterial blood pressure. Adenosine addition to cardioplegic solutions used in cardiac operations is clinically well tolerated and has been shown to improve myocardial protection in several studies. However, the mechanism of action remains unclear. Therefore, it is important to define the effect of adenosine on the inflammatory cascade as immune cell activation occurs early during ischemia reperfusion injury. Adenosine appears to mediate the initial steps of the inflammatory cascade via its four G-coupled protein receptors: A1, A2A, A2B, and A3, expressed on neutrophils, lymphocytes and macrophages. The adenosine receptor isotype dictates the immune response. More specifically, the A1 and A3 receptors stimulate a pro-inflammatory immune response whereas the A2A and A2B are immunosuppressive. As the adenosine receptors are important for cardiac pre-conditioning and post-conditioning, adenosine may regulate the inflammatory responses initiated during ischemia-mediated immune injury related to myocardial protection.

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