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Enhanced Activity by NKCC1 and Slc26a6 Mediates Acidic pH and Cl− Movement after Cardioplegia-Induced Arrest of db/db Diabetic Heart

机译：db / db糖尿病心脏引起的心脏停搏后NKCC1和Slc26a6增强的活性介导酸性pH和Cl−运动

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Diabetic heart dysfunctions during cardiac surgeries have revealed several clinical problems associated with ion imbalance. However, the mechanism of ion imbalance mediated by cardioplegia and a diabetic heart is largely unclear. We hypothesized that ion transporters might be regulated differently in the diabetic heart and that the differentially regulated ion transporters may involve in ion imbalance of the diabetic heart after cardioplegic arrest. In this study, we modified the Langendorff-free cardioplegia method and identified the involved ion transporters after cardioplegia-induced arrest between wild type and db/db heart. Enhanced expression of Na⁺-K⁺-2Cl⁻ cotransporter 1 (NKCC1) was observed in the db/db heart compared to the wild type heart. Enhanced NKCC1 activity was observed in the left ventricle of db/db mice compared to that of wild type after cardioplegia-induced arrest. The expression and activity of Slc26a6, a dominant Cl⁻/HCO3⁻ exchanger in cardiac tissues, were enhanced in left ventricle strips of db/db mice compared to that of wild type. The Cl⁻ transporting activity in left ventricle strips of db/db mice was dramatically increased as compared to that of wild type. Interestingly, expression of Slc26a6, as well as carbonic anhydrase IV as a supportive enzyme of Slc26a6, was increased in db/db cardiac strips compared to wild type cardiac strips. Thus, the enhanced Cl⁻ transporting activity and expression by NKCC1 and Slc26a6 in db/db cardiac tissues after cardioplegia-induced arrest provide greater insight into enhanced acidosis and Cl⁻ movement-mediated db/db heart dysfunction. Thus, we suggested that enhanced Cl⁻ influx and HCO3⁻ efflux through NKCC1 and Slc26a6 offer more acidic circumstances in the diabetic heart after cardioplegic arrest. These transporters should be considered as potential therapeutic targets to develop the next generation of cardioplegia solution for protection against ischemia-reperfusion injury in diabetic hearts.

机译：心脏外科手术期间的糖尿病性心脏功能障碍已揭示出一些与离子失衡有关的临床问题。然而，由心脏停搏和糖尿病性心脏介导的离子失衡的机制在很大程度上尚不清楚。我们假设在糖尿病心脏中离子转运蛋白可能受到不同的调节，而在心脏停搏后，差异调节的离子转运蛋白可能与糖尿病心脏的离子失衡有关。在这项研究中，我们修改了无Langendorff的心脏停搏方法，并确定了心脏停停引起的野生型和db / db心脏停搏后所涉及的离子转运蛋白。与野生型相比，在db / db心脏中观察到Na ^{+ -K ^{+ -2Cl ^{-共转运蛋白1（NKCC1）的增强表达心。在心脏停搏诱发的停搏后，与野生型相比，在db / db小鼠的左心室中观察到了增强的NKCC1活性。与野生型相比，db / db小鼠左心室条带中Scl26a6（一种主要的Cl ^{- / HCO3 ^{-交换子）在心脏组织中的表达和活性增强。。与野生型相比，db / db小鼠左心室条带的Cl ^{-转运活性显着增加。有趣的是，与野生型心脏试纸条相比，db / db心脏试纸条中Slc26a6的表达以及碳酸酐酶IV作为Slc26a6的支持酶都增加了。因此，心脏停搏诱发的停搏后db / db心脏组织中NKCC1和Slc26a6增强的Cl ^{-转运活性和表达，为增强酸中毒和Cl ^{-运动提供了更深入的了解。介导的db / db心脏功能障碍。因此，我们建议在心脏停搏后，通过NKCC1和Slc26a6增强的Cl ^{-内流和HCO3 ^{-外排提供了更多的酸性环境。这些转运蛋白应被视为开发下一代心脏停搏液的潜在治疗靶标，以保护糖尿病心脏免于缺血再灌注损伤。}}}}}}}}}}

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期刊名称 Mediators of Inflammation
作者
Minjeong Ji; Seok In Lee; Sang Ah Lee; Kuk Hui Son; Jeong Hee Hong;
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年(卷),期 2019(2019),-1
年度 2019
页码 7583760
总页数 12
原文格式 PDF
正文语种
中图分类细胞生物学;免疫学;
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1. Enhanced Activity by NKCC1 and Slc26a6 Mediates Acidic pH and Cl? Movement after Cardioplegia-Induced Arrest of db/db Diabetic Heart [J] . Minjeong Ji, Seok In Lee, Sang Ah Lee, Mediators of inflammation . 2019,第5期

机译：NKCC1和SLC26A6的增强活性介导酸性pH和CL？心脏停搏后的运动诱导诱导DB / DB糖尿病心脏
2. What are the biochemical mechanisms responsible for enhanced fatty acid utilization by perfused hearts from type 2 diabetic db/db mice? [J] . Carley AN, Severson DL Cardiovascular drugs and therapy . 2008,第2期

机译：2型糖尿病db / db小鼠灌注心脏增强脂肪酸利用的生化机制是什么？
3. What are the Biochemical Mechanisms Responsible for Enhanced Fatty Acid Utilization by Perfused Hearts from Type 2 Diabetic db/db Mice? [J] . Andrew N. Carley, David L. Severson Cardiovascular Drugs and Therapy . 2008,第2期

机译：2型糖尿病db / db小鼠的灌注心脏负责增强脂肪酸利用的生化机制是什么？
4. IN SITU TISSUE ENGINEERING USING ANGIOGENIC NANOSCAFFOLD ENHANCES DIABETIC WOUND HEALING IN DB/DB MOUSE MODEL [C] . Swathi Balaji, Sachin S. Vaikunth, Jignesh K. Parvadia, ASME summer bioengineering conference;SBC2008 . 2009

机译：使用血管生成纳米支架的原位组织工程增强了DB / DB小鼠模型中的糖尿病伤口愈合
5. Acidic phospholipid deficiency results in an inhibition of chromosomal replication and cell-cycle specific arrest in Escherichia coli. [D] . Fingland, Nicholas K. 2012

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6. Huangqi-Danshen decoction alleviates diabetic nephropathy in db/db mice by inhibiting PINK1/Parkin-mediated mitophagy [O] . Xinhui Liu, Jiandong Lu, Siqi Liu, 2020

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7. Enhanced Activity by NKCC1 and Slc26a6 Mediates Acidic pH and Cl− Movement after Cardioplegia-Induced Arrest of db/db Diabetic Heart [O] . Minjeong Ji, Seok In Lee, Sang Ah Lee, 2019

机译：NKCC1和SLC26A6的增强活性介导酸性pH和CL-运动诱导的DB / DB糖尿病心脏
8. Guidance for the Reregistration of Pesticide Products Containing 4-(2,4-Dichlorophenoxy) Butyric Acid (2,4-DB) and Its Salt, Amine and Esters as the Active Ingredient [R] . 1988

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Enhanced Activity by NKCC1 and Slc26a6 Mediates Acidic pH and Cl− Movement after Cardioplegia-Induced Arrest of db/db Diabetic Heart

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