Short-term hypoxia (5 h) in cultured neonatal rat ventricular myocytes decreased total Cx43 protein by 50% and conduction velocity by approximately 20% compared to normoxic cultures.
Short-term hypoxia decreases Cx43 protein and conduction velocity in cultured neonatal rat ventricular myocytes, contributing to the generation of an arrhythmogenic substrate.
OBJECTIVES: Altered gap junctional coupling of ventricular myocytes plays an important role in arrhythmogenesis in ischemic heart disease. Since hypoxia is a major component of ischemia, we tested the hypothesis that hypoxia causes gap junctional remodeling accompanied by conduction disturbances. METHODS: Cultured neonatal rat ventricular myocytes were exposed to hypoxia (1% O(2)) for 15 min to 5 h, connexin43 (Cx43) expression was analyzed, and conduction velocity was measured using the Micro-Electrode Array data acquisition system. RESULTS: After 15 min of hypoxia, conduction velocity was unaffected, while total Cx43, including the phosphorylated and nonphosphorylated isoforms, was increased. After 5 h of hypoxia, total Cx43 protein was decreased by 50%, while the nonphosphorylated Cx43 isoform was unchanged. Confocal analyses yielded a 55% decrease in the gap junctional Cx43 fluorescence signal, a 55% decrease in gap junction number, and a 26% decrease in size. The changes in Cx43 were not accompanied by changes in mRNA levels. The reduction in Cx43 protein levels was associated with a approximately 20% decrease in conduction velocity compared to normoxic cultures. CONCLUSIONS: Short-term hypoxia (5 h) decreases Cx43 protein and conduction velocity, thereby contributing to the generation of an arrhythmogenic substrate.
Zeevi‐Levin et al. (Tue,) conducted a other in ischemic heart disease. Hypoxia vs. normoxic cultures was evaluated on Cx43 expression and conduction velocity. Short-term hypoxia (5 h) in cultured neonatal rat ventricular myocytes decreased total Cx43 protein by 50% and conduction velocity by approximately 20% compared to normoxic cultures.
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