Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice

© 2018 Elsevier Ltd Although disturbance of cardiac Ca2+regulation is involved in the pathophysiology of iron-overload cardiomyopathy, the obvious mechanisms involved in the dysregulation of iron-induced cardiac Ca2+are unclear. Moreover, the roles of the iron chelator deferiprone and the T-type cal...

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Main Authors: Juthamas Khamseekaew, Sirinart Kumfu, Siripong Palee, Suwakon Wongjaikam, Somdet Srichairatanakool, Suthat Fucharoen, Siriporn C. Chattipakorn, Nipon Chattipakorn
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Published: 2018
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spelling th-cmuir.6653943832-582432018-09-05T04:21:33Z Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice Juthamas Khamseekaew Sirinart Kumfu Siripong Palee Suwakon Wongjaikam Somdet Srichairatanakool Suthat Fucharoen Siriporn C. Chattipakorn Nipon Chattipakorn Biochemistry, Genetics and Molecular Biology © 2018 Elsevier Ltd Although disturbance of cardiac Ca2+regulation is involved in the pathophysiology of iron-overload cardiomyopathy, the obvious mechanisms involved in the dysregulation of iron-induced cardiac Ca2+are unclear. Moreover, the roles of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac intracellular Ca2+transients and Ca2+regulatory proteins in thalassemic mice are still unknown. We tested the hypothesis that treatment with either deferiprone or efonidipine attenuated cardiac Ca2+dysregulation and led to improved left ventricular (LV) function in iron-overloaded thalassemic mice. Wild-type (WT) mice and β-thalassemic (HT) mice were fed with either a normal diet (ND) or a high iron-diet (FE) for 90 days. Then, the FE-fed mice were treated with either deferiprone (75 mg/kg/day) or efonidipine (4 mg/kg/day) for 30 days. ND-fed HT mice had an increase in T-type calcium channels (TTCC) and an increased level of sarcoplasmic reticulum Ca2+-ATPase (SERCA), compared with ND-fed WT mice. Chronic iron feeding led to an increase in TTCC and expression of SERCA proteins in FE-fed WT mice. Moreover, chronic iron overload led to increased plasma non-transferrin bound iron (NTBI) and cardiac iron deposition, impaired cardiac intracellular Ca2+transients including decreased intracellular Ca2+transient amplitude, rising rate and decay rate, as well as impaired LV function as indicated by a decreased %LV ejection fraction (%LVEF) in both WT and HT mice. Our findings showed that treatment with either deferiprone (DFP) or efonidipine (EFO) showed similar benefits in reducing plasma NTBI and cardiac iron deposition, and improving %LVEF from 84.3 (WT) to 89.3 (DFP) and 89.2 (EFO) treatment; and from 84.2 (HT) to 88.8 (DFP) and 89.5 (EFO) treatment, however there was no improvement in the regulation of cardiac Ca2+in iron-overloaded thalassemic mice. These findings provide the understanding of the effects of these drugs on the iron-overloaded heart in thalassemic mice and suggest that an alternative intervention that could improve calcium regulation under this condition is needed to improve the therapeutic outcome. Moreover, whether the benefits of the TTCC blocker is via its inhibition of the TTCC alone or together with its ability to chelate iron are still unclear and need further investigation. 2018-09-05T04:21:33Z 2018-09-05T04:21:33Z 2018-06-01 Journal 15321991 01434160 2-s2.0-85044378999 10.1016/j.ceca.2018.01.004 https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85044378999&origin=inward http://cmuir.cmu.ac.th/jspui/handle/6653943832/58243
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
topic Biochemistry, Genetics and Molecular Biology
spellingShingle Biochemistry, Genetics and Molecular Biology
Juthamas Khamseekaew
Sirinart Kumfu
Siripong Palee
Suwakon Wongjaikam
Somdet Srichairatanakool
Suthat Fucharoen
Siriporn C. Chattipakorn
Nipon Chattipakorn
Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
description © 2018 Elsevier Ltd Although disturbance of cardiac Ca2+regulation is involved in the pathophysiology of iron-overload cardiomyopathy, the obvious mechanisms involved in the dysregulation of iron-induced cardiac Ca2+are unclear. Moreover, the roles of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac intracellular Ca2+transients and Ca2+regulatory proteins in thalassemic mice are still unknown. We tested the hypothesis that treatment with either deferiprone or efonidipine attenuated cardiac Ca2+dysregulation and led to improved left ventricular (LV) function in iron-overloaded thalassemic mice. Wild-type (WT) mice and β-thalassemic (HT) mice were fed with either a normal diet (ND) or a high iron-diet (FE) for 90 days. Then, the FE-fed mice were treated with either deferiprone (75 mg/kg/day) or efonidipine (4 mg/kg/day) for 30 days. ND-fed HT mice had an increase in T-type calcium channels (TTCC) and an increased level of sarcoplasmic reticulum Ca2+-ATPase (SERCA), compared with ND-fed WT mice. Chronic iron feeding led to an increase in TTCC and expression of SERCA proteins in FE-fed WT mice. Moreover, chronic iron overload led to increased plasma non-transferrin bound iron (NTBI) and cardiac iron deposition, impaired cardiac intracellular Ca2+transients including decreased intracellular Ca2+transient amplitude, rising rate and decay rate, as well as impaired LV function as indicated by a decreased %LV ejection fraction (%LVEF) in both WT and HT mice. Our findings showed that treatment with either deferiprone (DFP) or efonidipine (EFO) showed similar benefits in reducing plasma NTBI and cardiac iron deposition, and improving %LVEF from 84.3 (WT) to 89.3 (DFP) and 89.2 (EFO) treatment; and from 84.2 (HT) to 88.8 (DFP) and 89.5 (EFO) treatment, however there was no improvement in the regulation of cardiac Ca2+in iron-overloaded thalassemic mice. These findings provide the understanding of the effects of these drugs on the iron-overloaded heart in thalassemic mice and suggest that an alternative intervention that could improve calcium regulation under this condition is needed to improve the therapeutic outcome. Moreover, whether the benefits of the TTCC blocker is via its inhibition of the TTCC alone or together with its ability to chelate iron are still unclear and need further investigation.
format Journal
author Juthamas Khamseekaew
Sirinart Kumfu
Siripong Palee
Suwakon Wongjaikam
Somdet Srichairatanakool
Suthat Fucharoen
Siriporn C. Chattipakorn
Nipon Chattipakorn
author_facet Juthamas Khamseekaew
Sirinart Kumfu
Siripong Palee
Suwakon Wongjaikam
Somdet Srichairatanakool
Suthat Fucharoen
Siriporn C. Chattipakorn
Nipon Chattipakorn
author_sort Juthamas Khamseekaew
title Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
title_short Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
title_full Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
title_fullStr Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
title_full_unstemmed Effects of the iron chelator deferiprone and the T-type calcium channel blocker efonidipine on cardiac function and Ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
title_sort effects of the iron chelator deferiprone and the t-type calcium channel blocker efonidipine on cardiac function and ca<sup>2+</sup>regulation in iron-overloaded thalassemic mice
publishDate 2018
url https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85044378999&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/58243
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