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Immediate-early gene induction and MAP kinase activation during recovery from metabolic inhibition in cultured cardiac myocytes.

机译：从培养心肌心肌细胞的代谢抑制恢复过程中立即早期基因诱导和MAP激酶激活。

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To investigate how cardiac myocytes recover from a brief period of ischemia, we used a metabolic inhibition (MI) model, one of the in vitro ischemic models, of chick embryo ventricular myocytes, and examined the induction of immediate-early (IE) genes mRNAs and the activity of mitogen-activated protein (MAP) kinase. We performed Northern blot analysis to study the expression of c-jun, c-fos, and c-myc mRNAs during MI using 1 mM NaCN and 20 mM 2-deoxy-d-glucose, and also during the recovery from MI of 30 min. The c-fos mRNA was induced transiently at 30 and 60 min during the recovery. The expression of c-jun mRNA was significantly augmented at 30, 60, 90, and 120 min during the recovery (3.0-, 4.7-, 2.4-, and 1.9-fold induction, respectively) and so did the expression of c-myc mRNA (1.4-, 1.7-, 1.8-, and 2.0-fold induction, respectively). In contrast, the levels of these mRNAs remained unchanged during MI. The electrophoretic mobility shift assay revealed that AP-1 DNA binding activity markedly increased at 120 min during the recovery. When the cells were pretreated with protein kinase C (PKC) inhibitors, 100 microM H-7 or 1 microM staurosporine, the induction of c-jun mRNA at 60 min during the recovery was markedly suppressed (95 or 82% reduction, respectively). The c-jun induction was partially inhibited when the cells were treated with 2 mM EGTA during MI and the recovery (42% reduction). MAP kinase activity quantified with in-gel kinase assay was unchanged during MI, but significantly increased at 5, 10, and 15 min during the recovery (3.0-, 4.1-, and 3.4-fold increase, respectively). S6 kinase activity was also augmented significantly at 15 min during the recovery. Thus, these data suggest that IE genes as well as MAP kinase may play roles in the recovery process of cardiac myocytes from MI, and that the augmentation of c-jun expression needs the activation of PKC and to some extent, [Ca2+]i.

机译：为了研究心肌细胞如何从短暂的缺血中恢复，我们使用了一种代谢抑制（MI）模型（一种体外缺血模型），对鸡胚心室肌细胞进行了研究，并研究了即早（IE）基因mRNA的诱导和有丝分裂原激活蛋白（MAP）激酶的活性。我们进行了Northern印迹分析，以研究使用1 mM NaCN和20 mM 2-脱氧-d-葡萄糖在心梗期间以及从心梗恢复30分钟期间c-jun，c-fos和c-myc mRNA的表达。。恢复过程中，在30和60分钟时瞬时诱导了c-fos mRNA。恢复过程中，在30、60、90和120分钟时，c-jun mRNA的表达显着增加（分别是诱导的3.0倍，4.7倍，2.4倍和1.9倍），c-myc的表达也如此。 mRNA（分别为1.4倍，1.7倍，1.8倍和2.0倍诱导）。相反，在心梗期间这些mRNA的水平保持不变。电泳迁移率变动分析表明，恢复期间120分钟时AP-1 DNA结合活性显着增加。当用蛋白激酶C（PKC）抑制剂，100 microM H-7或1 microM星形孢菌素预处理细胞时，恢复过程中60分钟时c-jun mRNA的诱导被显着抑制（分别降低95％或82％）。当在MI和恢复期间用2 mM EGTA处理细胞时，c-jun诱导被部分抑制（减少42％）。用凝胶内激酶测定定量的MAP激酶活性在MI期间没有变化，但在恢复过程的第5、10和15分钟显着增加（分别增加了3.0倍，4.1倍和3.4倍）。恢复期间15分钟时S6激酶活性也显着增强。因此，这些数据表明，IE基因以及MAP激酶可能在心肌细胞从MI的恢复过程中发挥作用，并且c-jun表达的增强需要PKC的激活，并在某种程度上需要[Ca2 +] i。

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期刊名称 The Journal of Clinical Investigation
作者
A Yao; T Takahashi; T Aoyagi; K Kinugawa; O Kohmoto; S Sugiura; T Serizawa;
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年(卷),期 1995(96),1
年度 1995
页码 69–77
总页数 9
原文格式 PDF
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中图分类医学史;
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入库时间 2022-08-17 11:56:00

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2. Regulated expression of a contractile protein gene correlates with recovery of contractile function after reversible metabolic inhibition in cultured myocytes. [J] . Barry WH, Hamilton CA, Knowlton KU Journal of Molecular and Cellular Cardiology . 1995,第1期

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3. Two distinct mechanisms of angiotensin II-induced negative regulation of the mitogen-activated protein kinases in cultured cardiac myocytes. [J] . Hiroi Y, Hiroi J, Kudoh S, Hypertension research: Official journal of the Japanese Society of Hypertension . 2001,第4期

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Immediate-early gene induction and MAP kinase activation during recovery from metabolic inhibition in cultured cardiac myocytes.

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