Leptin attenuates cardiac apoptosis after chronic ischaemic injury

doi:10.1093/cvr/cvp071

Cardiovascular Research Advance Access first published online on February 20, 2009
This version [Corrected Proof] published online on March 17, 2009
Cardiovascular Research, doi:10.1093/cvr/cvp071

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Leptin attenuates cardiac apoptosis after chronic ischaemic injury

Kenneth R. McGaffin¹^,*, Baobo Zou², Charles F. McTiernan¹ and Christopher P. O’Donnell²

¹ Cardiovascular Institute, University of Pittsburgh Medical Center, 1750 Bioscience Tower, 200 Lothrop Street, Pittsburgh, PA 15213, USA
² Division of Pulmonary, Allergy, and Critical Care Medicine, University of Pittsburgh Medical Center, Pittsburgh, PA, USA

^* Corresponding author. Tel: +1 412 647 2345; fax: +1 412 383 8857. E-mail address: mcgaffinkr{at}upmc.edu

Aims: We have previously shown that activation of leptin signallingin the heart reduces cardiac morbidity and mortality after myocardialinfarction (MI). In the present study, we tested the hypothesisthat leptin signalling limits cardiac apoptosis after MI throughactivation of signal transducer and activator of transcription(STAT)-3 responsive anti-apoptotic genes, including B-cell lymphoma(bcl)-2 and survivin, that serve to downregulate the activityof caspase-3.

Methods and results: Hearts from C57BL/6J and three groups of leptin-deficient Ob/Obmice (food-restricted, ad libitum, and leptin-repleted) wereexamined 4 weeks after permanent left coronary artery ligationor sham operation. Inflammatory and apoptotic cell number wasdetermined in cardiac sections by immunostaining. Expressionof cardiac bcl-2, survivin, and pro and active caspase-3 wasdetermined and correlated with in vitro caspase-3 activity.In the absence of MI, both lean and obese leptin-deficient miceexhibited increased cardiac apoptosis compared with wild-typemice. After MI, the highest rates of apoptosis were seen inthe infarcted tissue of lean and obese Ob/Ob mice. Further,leptin-deficient hearts, as well as hearts from wild-type micetreated with the STAT-3 inhibitor WP1066, exhibited bluntedanti-apoptotic bcl-2 and survivin gene expression, and increasedcaspase-3 protein expression and activity. The increased caspase-3activity and apoptosis in hearts of leptin-deficient mice afterMI was significantly attenuated in Ob/Ob mice replete with leptin,reducing apoptosis to levels comparable to that observed inwild-type mice after MI.

Conclusion: These results demonstrate that intact leptin signalling post-MIacts through STAT-3 to increase anti-apoptotic bcl-2 and survivingene expression and reduces caspase-3 activity, consistent witha cardioprotective role of leptin in the setting of chronicischaemic injury.

KEYWORDS Apoptosis; Leptin; Survivin; bcl-2; Heart failure

Time for primary review: 30 days

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