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α2钠泵同工型的相对丰度影响小鼠心室肌细胞中的钠钙交换电流和钙瞬变。

Relative abundance of alpha2 Na(+) pump isoform influences Na(+)-Ca(2+) exchanger currents and Ca(2+) transients in mouse ventricular myocytes.

作者信息

Yamamoto Taku, Su Zhi, Moseley Amy E, Kadono Toshie, Zhang John, Cougnon Marc, Li Fenghua, Lingrel Jerry B, Barry William H

机构信息

Cardiology Division, University of Utah Health Sciences Center, 50 North Medical Drive, Salt Lake City, UT 84132, USA.

出版信息

J Mol Cell Cardiol. 2005 Jul;39(1):113-20. doi: 10.1016/j.yjmcc.2005.03.023.

Abstract

In the mouse, genetic reduction in the Na(+), K(+)-ATPase alpha1 or alpha2 isoforms results in different functional phenotypes: heterozygous alpha2 isolated hearts are hypercontractile, whereas heterozygous alpha1 hearts are hypocontractile. We examined Na(+)/Ca(2+) exchange (NCX) currents in voltage clamped myocytes (pipette [Na(+)]=15 mM) induced by abrupt removal of extracellular Na(+). In wild-type (WT) myocytes, peak exchanger currents were 0.59+/-0.04 pA/pF (mean+/-S.E.M., n=10). In alpha1(+/-) myocytes (alpha2 isoform increased by 54%), NCX current was reduced to 0.33+/-0.05 (n=9, P<0.001) indicating a lower subsarcolemmal [Na(+)]. In alpha2(+/-) myocytes (alpha2 isoform reduced by 54%), the NCX current was increased to 0.89+/-0.11 (n=8, P=0.03). The peak sarcolemmal Na(+) pump currents activated by abrupt increase in K(+) to 4 mM in voltage clamped myocytes in which the Na(+) pump had been completely inhibited for 5 min by exposure to 0 K(+) were similar in alpha1(+/-) (0.86+/-0.12, n=10) and alpha2(+/-) myocytes (0.94+/-0.08 pA/pF, n=16), and were slightly but insignificantly reduced relative to WT (1.03+/-0.05, n=24). The fluo-3 Ca(2+) transient (F/F(o)) in WT myocytes paced at 0.5 Hz was 2.18+/-0.09, n=34, was increased in alpha2(+/-) myocytes (F/F(o)=2.56+/-0.14, n=24, P=0.02), and was decreased in alpha1(+/-) myocytes (F/F(o)=1.93+/-0.08, n=28, P<0.05). Thus the alpha2 isoform rather than the alpha1 appears to influence Na(+)/Ca(2+) exchanger currents Ca(2+) transients, and contractility. This finding is consistent with the proposal that alpha2 isoform of the Na pump preferentially alters [Na(+)] in a subsarcolemmal micro-domain adjacent to Na(+)/Ca(2+) exchanger molecules and SR Ca(2+) release sites.

摘要

在小鼠中,Na(+)、K(+)-ATP酶α1或α2亚型的基因表达降低会导致不同的功能表型:杂合α2型离体心脏收缩增强,而杂合α1型心脏收缩减弱。我们检测了在电压钳制的心肌细胞(移液管内[Na(+)] = 15 mM)中,通过突然去除细胞外Na(+)所诱导的Na(+)/Ca(2+)交换(NCX)电流。在野生型(WT)心肌细胞中,交换电流峰值为0.59±0.04 pA/pF(平均值±标准误,n = 10)。在α1(+/-)心肌细胞(α2亚型增加54%)中,NCX电流降至0.33±0.05(n = 9,P<0.001),表明肌膜下[Na(+)]较低。在α2(+/-)心肌细胞(α2亚型减少54%)中,NCX电流增加至0.89±0.11(n = 8,P = 0.03)。在电压钳制的心肌细胞中,通过将K(+)突然增加到4 mM激活的肌膜Na(+)泵电流峰值,在α1(+/-)(0.86±0.12,n = 10)和α2(+/-)心肌细胞(0.94±0.08 pA/pF,n = 16)中相似,相对于WT(1.

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