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Publication Details
AFRICAN RESEARCH NEXUS
SHINING A SPOTLIGHT ON AFRICAN RESEARCH
biochemistry, genetics and molecular biology
Dual activation of STAT-3 and Akt is required during the trigger phase of ischaemic preconditioning
Cardiovascular Research, Volume 79, No. 1, Year 2008
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Description
Aims: During preconditioning by tumour necrosis factor-α (TNFα), activation of the signal transducer and activator of transcription-3 (STAT-3) but not Akt, is essential, whereas ischaemic cardiac preconditioning (IPC) requires both STAT-3 and Akt at the time of reperfusion. However, it is not known whether the same signalling pattern occurs during the preconditioning stimulus (trigger phase) and whether links exist between STAT-3 and Akt. Hence, our hypothesis is that concomitant activation or co-interaction between these two key signals is required during the trigger phase for IPC. Conversely, we proposed that there would be no such interaction when preconditioning was induced by TNFα (TNF-PC). Methods and results: Cardiomyocytes, isolated from adult wild-type (WT) and cardiac-specific STAT-3 knockout (KO) mice, were exposed to simulated ischaemia (SI) reperfusion. Cells were preconditioned either by 30 min SI or by 30 min TNFα (0.5 ng/mL) in the presence or absence of AG490 (100 nM) or wortmannin (100 nM) to inhibit STAT-3 or Akt, respectively. Cell viability was evaluated by trypan blue, and phosphorylation levels of STAT-3 and Akt were measured by Western blot analysis. Similar experiments were conducted in isolated rat hearts subjected to an ischaemia-reperfusion insult. Both preconditioning stimuli failed to protect KO cardiomyocytes, and addition of AG490 abolished preconditioning in WT cardiomyocytes or isolated hearts. Wortmannin abolished the protection afforded by IPC, but did not affect TNF-PC in both models. Western blot analysis demonstrated that added wortmannin during IPC stimulus decreased STAT-3 phosphorylation while, conversely, AG490 reduced Akt phosphorylation. Conclusion: STAT-3 activation could be achieved independent of Akt during TNF-PC. In contrast, during an IPC stimulus, both prosurvival signalling molecule cascades acted in concert so that inhibiting activation of STAT-3 also inhibited that of Akt and vice versa. © The Author 2008.
Authors & Co-Authors
Suleman, Naushaad
South Africa, Cape Town
University of Cape Town
Somers, Sarin J.
South Africa, Cape Town
University of Cape Town
Smith, Robert M.
South Africa, Cape Town
University of Cape Town
Opie, LionelH H.
South Africa, Cape Town
University of Cape Town
Lecour, Sandrine C.
South Africa, Cape Town
University of Cape Town
Statistics
Citations: 132
Authors: 5
Affiliations: 1
Identifiers
Doi:
10.1093/cvr/cvn067
ISSN:
00086363
e-ISSN:
17553245
Research Areas
Cancer
Noncommunicable Diseases