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NBCe1 Na+-HCO3-cotransporter ablation causes reduced apoptosis following cardiac ischemia-reperfusion injury in vivo

NBCe1 Na^+-HCO3^- cotransporter ablation causes reduced apoptosis following cardiac ischemia-reperfusion injury in vivo
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摘要 AIM To investigate the hypothesis that cardiomyocytespecific loss of the electrogenic NBCe1 Na^+-HCO3^- cotransporter is cardioprotective during in vivo ischemiareperfusion(IR)injury.METHODS An NBCe1 (Slc4a4 gene) conditional knockout mouse(KO)model was prepared by gene targeting.Cardiovascular performance of wildtype (WT) and cardiac-specific NBCe1 KO mice was analyzed by intraventricular pressure measurements,and changes in cardiac gene expression were determined by RNA Seq analysis.Response to in vivo IR injury was analyzed after 30 min occlusion of the left anterior descending artery followed by 3 h of reperfusion. RESULTS Loss of NBCe1 in cardiac myocytes did not impair cardiac contractility or relaxation under basal conditions or in response toβ-adrenergic stimulation,and caused only limited changes in gene expression patterns,such as those for electrical excitability.However,following ischemia and reperfusion,KO heart sections exhibited significantly fewer apoptotic nuclei than WT sections.CONCLUSION These studies indicate that cardiac-specific loss of NBCe1 does not impair cardiovascular performance,causes only minimal changes in gene expression patterns,and protects against IR injury in vivo. AIM To investigate the hypothesis that cardiomyocytespecific loss of the electrogenic NBCe1 Na^+-HCO3^- cotransporter is cardioprotective during in vivo ischemiareperfusion(IR)injury.METHODS An NBCe1 (Slc4a4 gene) conditional knockout mouse(KO)model was prepared by gene targeting.Cardiovascular performance of wildtype (WT) and cardiac-specific NBCe1 KO mice was analyzed by intraventricular pressure measurements,and changes in cardiac gene expression were determined by RNA Seq analysis.Response to in vivo IR injury was analyzed after 30 min occlusion of the left anterior descending artery followed by 3 h of reperfusion. RESULTS Loss of NBCe1 in cardiac myocytes did not impair cardiac contractility or relaxation under basal conditions or in response toβ-adrenergic stimulation,and caused only limited changes in gene expression patterns,such as those for electrical excitability.However,following ischemia and reperfusion,KO heart sections exhibited significantly fewer apoptotic nuclei than WT sections.CONCLUSION These studies indicate that cardiac-specific loss of NBCe1 does not impair cardiovascular performance,causes only minimal changes in gene expression patterns,and protects against IR injury in vivo.
出处 《World Journal of Cardiology》 CAS 2018年第9期97-109,共13页 世界心脏病学杂志(英文版)(电子版)
基金 Supported by NIH grants,No.HL061974(to Gary E Shull),No.R01HL136025(to Yigang Wang),No.P30ES006096(to Mario Medvedovic) funds from the Center for Clinical and Translational Science and Training,University of Cincinnati(to Gary E Shull) a Research Innovation Seed Grant from the University of Cincinnati(to Gary E Shull and John N Lorenz)
关键词 Deep SEQUENCING ISCHEMIC APOPTOSIS Slc4a4 NBCe1 Deep sequencing Ischemic Apoptosis Slc4a4 NBCe1
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