Discovery of a new function of cyclooxygenase (COX)-2: COX-2 is a cardioprotective protein that alleviates ischemia/reperfusion injury and mediates the late phase of preconditioning

doi:10.1016/S0008-6363(02)00414-5

Cardiovascular Research 2002 55(3):506-519; doi:10.1016/S0008-6363(02)00414-5
© 2002 by European Society of Cardiology

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Discovery of a new function of cyclooxygenase (COX)-2: COX-2 is a cardioprotective protein that alleviates ischemia/reperfusion injury and mediates the late phase of preconditioning

Roberto Bolli^*, Ken Shinmura, Xian-Liang Tang, Eitaro Kodani, Yu-Ting Xuan, Yiru Guo and Buddhadeb Dawn

Division of Cardiology, University of Louisville, and Jewish Hospital Heart and Lung Institute, 550 South Jackson St., Louisville, KY 40202, USA

^* Corresponding author. Tel.: +1-502-852-1837; fax: +1-502-852-6474 rbolli{at}louisville.edu

More than 10 years after its discovery, the function of cyclooxygenase-2(COX-2) in the cardiovascular system remains largely an enigma.Many scholars have assumed that the allegedly detrimental effectsof COX-2 in other systems (e.g. proinflammatory actions andtumorigenesis) signify a detrimental role of this protein incardiovascular homeostasis as well. This view, however, is ill-founded.Recent studies have demonstrated that ischemic preconditioning(PC) upregulates the expression and activity of COX-2 in theheart, and that this increase in COX-2 activity mediates theprotective effects of the late phase of PC against both myocardialstunning and myocardial infarction. An obligatory role of COX-2has been observed in the setting of late PC induced not onlyby ischemia but also by ${delta}$ -opioid agonists and physical exercise,supporting the view that the recruitment of this protein isa central mechanism whereby the heart protects itself from ischemia.The beneficial actions of COX-2 appear to be mediated by thesynthesis of PGE₂ and/or PGI₂. Since inhibition of iNOS in preconditionedmyocardium blocks COX-2 activity whereas inhibition of COX-2does not affect iNOS activity, COX-2 appears to be downstreamof iNOS in the protective pathway of late PC. The results ofthese studies challenge the widely accepted paradigm that viewsCOX-2 activity as detrimental. The discovery that COX-2 playsan indispensable role in the anti-stunning and anti-infarcteffects of late PC demonstrates that the recruitment of thisprotein is a fundamental mechanism whereby the heart adaptsto stress, thereby revealing a novel, hitherto unappreciatedcardioprotective function of COX-2. From a practical standpoint,the recognition that COX-2 is an obligatory co-mediator (togetherwith iNOS) of the protection afforded by late PC has implicationsfor the clinical use of COX-2 selective inhibitors as well asnonselective COX inhibitors. For example, the possibility thatinhibition of COX-2 activity may augment myocardial cell deathby obliterating the innate defensive response of the heart againstischemia/reperfusion injury needs to be considered and is theobject of much current debate. Furthermore, the concept thatthe COX-2 byproducts, PGE₂ and/or PGI₂, play a necessary rolein late PC provides a basis for novel therapeutic strategiesdesigned to enhance the biosynthesis of these cytoprotectiveprostanoids in the ischemic myocardium. From a conceptual standpoint,the COX-2 hypothesis of late PC expands our understanding ofthe function of this enzyme in the cardiovascular system andimpels a critical reassessment of current thinking regardingthe biologic significance of COX-2.

KEYWORDS Ischemia; Nitric oxide; Preconditioning; Reperfusion

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