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去铁胺可促进铁过载性心肌病沙鼠模型的存活并预防心电图异常。

Deferoxamine promotes survival and prevents electrocardiographic abnormalities in the gerbil model of iron-overload cardiomyopathy.

作者信息

Obejero-Paz Carlos A, Yang Tianen, Dong Wei-Qiang, Levy Matthew N, Brittenham Gary M, Kuryshev Yuri A, Brown Arthur M

机构信息

Rammelkamp Center for Education and Research, MetroHealth Campus, Cleveland, OH 44109, USA.

出版信息

J Lab Clin Med. 2003 Feb;141(2):121-30. doi: 10.1067/mlc.2003.18.

Abstract

We investigated the time course of electrocardiographic (ECG) changes in the Mongolian gerbil model of iron overload and the effects of the iron chelator deferoxamine (DFO) on these changes. Iron overload was produced with weekly subcutaneous injections of low doses (200 mg/kg/wk) or high doses (800 mg/kg/wk) of iron-dextran. DFO was administered subcutaneously at a dose of 200 mg/kg/day to high-dose animals. Our results show that (1) survival of iron-overloaded gerbils is dose-dependent, with median survival times of 68 and 14 weeks for low- and high-dose animals, respectively; (2) both low and high doses produce prolongation of the PR interval and bradycardia in early stages and prolongation of the QT interval, premature ventricular contractions, variable degrees of atrioventricular block, changes in the ST segment, and T-wave inversion at later stages coinciding with the development of heart failure; (3) DFO prevented death during 20 weeks of high-dose iron-dextran; (4) DFO prevented ECG changes, although delayed prolongation of PR intervals and QRS complexes occurred; and (5) despite marked prolongation of survival and prevention of ECG changes, DFO had modest effects on total cardiac iron content. We speculate that DFO chelates a small iron pool located within the cytoplasm of iron-overloaded cardiomyocytes.

摘要

我们研究了蒙古沙鼠铁过载模型中心电图(ECG)变化的时间进程以及铁螯合剂去铁胺(DFO)对这些变化的影响。通过每周皮下注射低剂量(200mg/kg/周)或高剂量(800mg/kg/周)的右旋糖酐铁来造成铁过载。以200mg/kg/天的剂量对高剂量组动物皮下注射DFO。我们的结果表明:(1)铁过载沙鼠的存活具有剂量依赖性,低剂量和高剂量组动物的中位生存时间分别为68周和14周;(2)低剂量和高剂量在早期均会导致PR间期延长和心动过缓,在后期随着心力衰竭的发展会出现QT间期延长、室性早搏、不同程度的房室传导阻滞、ST段改变和T波倒置;(3)DFO可防止高剂量右旋糖酐铁注射20周期间的死亡;(4)DFO可防止ECG变化,尽管PR间期和QRS波群出现延迟延长;(5)尽管生存时间显著延长且ECG变化得到预防,但DFO对心脏总铁含量的影响较小。我们推测DFO螯合了位于铁过载心肌细胞胞质内的一小部分铁池。

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