Ischemia Enhances Translocation of Connexin43 and Gap Junction Intercellular Communication, Thereby Propagating Contraction Band Necrosis After Reperfusion

Shintani-Ishida, Kaori; Unuma, Kana; Yoshida, Kenichi

doi:10.1253/circj.cj-09-0079

Cited by 29 publications

(29 citation statements)

References 40 publications

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“…27, 28 Heart homogenate was centrifuged at 1,000 × g for 10 min, and the supernatant was spun at 100,000 × g for 60 min. The 1,000 × g pellets, 100,000 × g pellets, and 100,000 × g supernatant are referred to as the P1, P2, and S fractions, respectively.…”

Section: Subcellular Fractionation and Western Blot Analysismentioning

confidence: 99%

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Connexin-43 Redistribution and Gap Junction Activation During Forced Restraint Protects Against Sudden Arrhythmic Death in Rats

Unuma

Shintani-Ishida

Tsushima

et al. 2010

Circ J

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Background: Connexin-43 (Cx43) expression is reduced or redistributed in heart disease. Restraint or other emotional stressors might cause sudden death in persons with such diseases, but the mechanism of death and its connection to Cx43 during restraint remain unknown. Whether Cx43 distribution or gap junction (GJ) function during restraint is involved in sudden arrhythmic death in rats is addressed in this study. Methods and Results:Male Sprague -Dawley rats underwent immobilization (IMO), and individual electrocardiographic responses were monitored by telemetry. Heart sections were used to examine ventricular Cx43 distribution, and GJ intercellular communication (GJIC) activity was assessed using a dye-transfer assay. IMO induced the translocation of Cx43 into to the GJ-rich fraction, with a peak at 60 min. During IMO, Cx43 immunofluorescence was enhanced at intercalated discs, in association with GJIC activation, and premature ventricular contractions (PVCs) increased. In the presence of the GJ inhibitor, carbenoxolone (0.25 mg·kg -1 ·h -1 ), IMO induced lethal ventricular tachycardia or fibrillation in 21.7% of rats, in association with QRS prolongation and increased PVCs.Conclusions: IMO causes Cx43 translocation to intercalated discs, thereby reducing vulnerability to lethal arrhythmias via enhancing GJ coupling. (Circ J 2010; 74: 1087 - 1095

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Section: Subcellular Fractionation and Western Blot Analysismentioning

confidence: 99%

“…28 GJIC was examined in pairs of rats, one of which underwent IMO + CBX for 60 min, while the other served as a control (free movement). Transverse sections were excised from the apexes.…”

Section: Dye Transfer Assay In Heart Sectionsmentioning

confidence: 99%

Connexin-43 Redistribution and Gap Junction Activation During Forced Restraint Protects Against Sudden Arrhythmic Death in Rats

Unuma

Shintani-Ishida

Tsushima

et al. 2010

Circ J

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“…10 Consistent with these reports, the authors also found that inhibition of enhanced GJIC ameliorated membrane disruption during reperfusion and reduced the CBN area and infarct size in the reperfused heart, providing in vivo evidence that gap junctions mediate the spread of cell death after ischemia-reperfusion injury (Figure 2). 6 In contrast to these results, many animal studies have demonstrated that ischemic insults induce rapid dephosphorylation of Cx43 and thereby alter the distribution of gap junctions from intercalated disks to the sides of cardiomyocytes (referred to as lateralization). 2,11 These alterations are thought to contribute to electrical uncoupling that provokes ventricular arrhythmia during myocardial ischemia.…”

Section: Article P 1661mentioning

confidence: 98%

“…In this issue of the Circulation Journal, Shintani-Ishida et al 6 examine the role of GJIC in ischemia-reperfusion injury. They carefully estimated cellular localization of phosphorylated and dephosphorylated Cx43 in the ischemic heart by using the subcellular fractionation technique.…”

Section: Article P 1661mentioning

confidence: 99%

Gap Junctions Mediate the Spread of Ischemia-Reperfusion Injury

Minamino

2009

Circ J

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“…There was no translocation of hypoxia inducible factor-1α, and the distribution of Cx43 was different from that in ischemia. 8 Unuma et al concluded that translocation of Cx43 to the GJ-enriched fraction occurs via the α1-adrenoceptor pathway independently of ischemia. 7 The results provided by Unuma et al 7 are the first demonstration of α-adrenoreceptor-dependent Cx43 translocation to GJs in IMO rats.…”

Section: Article P 2693mentioning

confidence: 99%

Does Remodeling of Gap Junctions and Connexin Expression Contribute to Arrhythmogenesis?

Hayashi

2010

Circ J

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Ischemia Enhances Translocation of Connexin43 and Gap Junction Intercellular Communication, Thereby Propagating Contraction Band Necrosis After Reperfusion

Cited by 29 publications

References 40 publications

Connexin-43 Redistribution and Gap Junction Activation During Forced Restraint Protects Against Sudden Arrhythmic Death in Rats

Connexin-43 Redistribution and Gap Junction Activation During Forced Restraint Protects Against Sudden Arrhythmic Death in Rats

Gap Junctions Mediate the Spread of Ischemia-Reperfusion Injury

Does Remodeling of Gap Junctions and Connexin Expression Contribute to Arrhythmogenesis?

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