INHIBITION OF MYOCARDIAL APOPTOSIS BY POSTCONDITIONING IS ASSOCIATED WITH ATTENUATION OF OXIDATIVE STRESS-MEDIATED NUCLEAR FACTOR-κκB TRANSLOCATION AND TNFαα RELEASE | Zendy

Hajime Kin | Zendy; Ning-Ping Wang | Zendy; James Mykytenko | Zendy; James G. Reeves | Zendy; Jeremiah Deneve | Zendy; Rong Jiang | Zendy; Amanda J. Zatta | Zendy; Robert A. Guyton | Zendy; Jakob VintenJohansen | Zendy; and Zhi-Qing Zhao | Zendy

Open Access

INHIBITION OF MYOCARDIAL APOPTOSIS BY POSTCONDITIONING IS ASSOCIATED WITH ATTENUATION OF OXIDATIVE STRESS-MEDIATED NUCLEAR FACTOR-κκB TRANSLOCATION AND TNFαα RELEASE

Author(s) -

Hajime Kin,

Ning-Ping Wang,

James Mykytenko,

James G. Reeves,

Jeremiah Deneve,

Rong Jiang,

Amanda J. Zatta,

Robert A. Guyton,

Jakob VintenJohansen,

and Zhi-Qing Zhao

Publication year - 2008

Publication title -

shock

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.095

H-Index - 117

eISSN - 1540-0514

pISSN - 1073-2322

DOI - 10.1097/shk.0b013e31815cfd5a

Subject(s) - malondialdehyde , oxidative stress , apoptosis , chemistry , superoxide , tumor necrosis factor alpha , pharmacology , chromosomal translocation , reperfusion injury , ischemia , medicine , endocrinology , biochemistry , enzyme , gene

Oxidative stress-stimulated nuclear factor-kappa B (NF-kappa B) activation has been associated with rapid transcription of TNF-alpha and induction of apoptosis. This study tested the hypothesis that postconditioning (Postcon) reduces myocardial apoptosis and inhibits translocation of NF-kappa B and release of TNF-alpha secondary to an attenuation of oxidant generation during reperfusion. Anesthetized rats were subjected to 30 min of ischemia and 3 h of reperfusion and divided randomly to Control or Postcon (three cycles of 10-s reperfusion and 10-s reocclusion applied at the onset of reperfusion) group, respectively. Relative to Control, Postcon reduced the plasma malondialdehyde (1.21 +/- 0.08 vs. 0.8 +/- 0.06* microM/mL) and decreased the generation of superoxide radical in area at risk myocardium (dihydroethidium staining). Compared with Control, Postcon also inhibited translocation of NF-kappa B to nuclei (167% +/- 21% vs. 142% +/- 18%*), decreased the level of plasma TNF-alpha (1,994 +/- 447 vs. 667 +/- 130* pg/mL), and inhibited caspase-3 activity (0.57% +/- 0.1% vs. 0.21% +/- 0.1%*). The number of apoptotic cells (percent total nuclei) in ischemic myocardium was reduced (20% +/- 1% vs. 11% +/- 2%*), consistent with reduced appearance of DNA fragmentation. To support whether oxidant generation is important in the triggering of cytokine release and apoptosis, N-acetylcysteine (NAC), a potent antioxidant agent, was administered before ischemia and at reperfusion. Treatment with NAC inhibited superoxide radical generation and decreased plasma malondialdehyde to a comparable level to that in Postcon, concomitant with an inhibition of NF-kappa B expression (42% +/- 8%*) and reduction of release of TNF-alpha (231 +/- 72* pg/mL). Caspase-3 activity (0.33% +/- 0.1%*) and apoptotic cells (12% +/- 1%*) were also comparably reduced by NAC. These data suggest that Postcon attenuates myocardial apoptosis, reduces caspase-3 activity, and is potentially mediated by inhibiting oxidant-activated NF-kappa B-TNF-alpha signaling pathway. *P < 0.05 Postcon and NAC vs. Control.

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