Isradipine prevents the development of spontaneously occurring cardiac necrosis in cardiomyopathic hamster

Jacques, Danielle; Bkaily, Ghassan; Jasmin, G.; D’Orléans-Juste, Pedro; Chahine, Mirna

doi:10.1139/y03-021

Cited by 7 publications

(8 citation statements)

References 25 publications

(38 reference statements)

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“…These results suggest that HF leading to early death of HCMHs is not fully due to the increase in NHE-1 density. As was previously suggested, the EMD-insensitive increase in necrosis as well as increases in [Na + ] i and [Ca 2+ ] i could be due in part to the continual presence of the slow sodium channel (Bkaily and Jacques 1994;Jacques et al 2003) and a decrease in the expression of cardiac Na + -K + ATPase (Watanabe et al 1998). However, EMD completely prevented the development of hypertrophy and HF as well as the increase in NHE-1 density, in addition to preventing the premature death of HCMHs.…”

Section: Discussionmentioning

confidence: 64%

“…Longitudinal sectioning of the heart (at least 30 sections) permits a good quantitative assessment of the lesions throughout the heart (Chahine et al 2005). Serial 5 m paraffin sections were stained with hematoxylin-phloxine-saffron Proschek 1984, 1994;Jacques et al 2003;Chahine et al 2005). Von Kossa's silver staining method was used to estimate myocardial calcification Chahine et al 2005).…”

Section: Histopathological Studiesmentioning

confidence: 99%

“…As described previously (Jasmin and Proschek 1984;Jacques et al 2003;Chahine et al 2005), necrosis was measured using a double-blind procedure and an arbitrary scale of 0-3 (Jasmin and Proschek 1984;Jacques et al 2003;Chahine et al 2005). A maximum score of 3.0 indicates that the damage exceeded 50%, whereas lower scores correspond to moderate and mild severity changes Proschek 1984, 1994;Chahine et al 2005).…”

Section: Histopathological Studiesmentioning

confidence: 99%

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Na⁺–H⁺ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Bkaily

Chahine

Al-Khoury

et al. 2015

Can. J. Physiol. Pharmacol.

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Using the UM-X7.1 hereditary cardiomyopathic and muscular dystrophy hamsters (HCMH), we tested the effects of lifelong preventive or curative treatments during the heart failure phase with the NHE-1 inhibitor EMD 87580 (EMD) or with the angiotensin-converting enzyme inhibitor cilazapril on the intracellular Na + and Ca 2+ overloads, elevated level of NHE-1, necrosis, hypertrophy, heart failure, and early death. Our results showed that 310-day pretreatment of 30-day-old HCMHs with EMD significantly prevented cardiac necrosis, cardiomyocyte hypertrophy, and reduced the heart to body mass ratio. This treatment significantly prevented Na + and Ca 2+ overloads and the increase in NHE-1 protein level observed in HCMHs. Importantly, this lifelong preventive treatment significantly decreased the levels of creatine kinase and prevented early death of HCMHs. Curative treatment of hypertrophic 275-day-old HCMHs for 85 days with EMD significantly prevented hypertrophy and early death of HCMHs. However, treatments with cilazapril did not have any significant effects on the cardiac parameters studied or on early death of HCMHs. Our results suggest that the increase in the NHE-1 level and the consequent Na + and Ca 2+ overloads are implicated in the pathological process leading to heart failure and early death in HCMHs, and treatment with the NHE-1 inhibitor is promising for preventing early death in hereditary cardiomyopathy.

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Section: Discussionmentioning

confidence: 64%

Section: Histopathological Studiesmentioning

confidence: 99%

Section: Histopathological Studiesmentioning

confidence: 99%

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Na⁺–H⁺ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Bkaily

Chahine

Al-Khoury

et al. 2015

Can. J. Physiol. Pharmacol.

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“…1), intracellular sodium overload (Fig. 2) is one of the earliest pathological signs (Bkaily et al , 2017Chahine et al 2005;Jacques et al 2003). The latter was found to be, in part, a consequence of the development of intracellular acidosis and the resulting sodium influx via the Na + -H + exchanger NHE-1 (Fig.…”

Section: Introductionmentioning

confidence: 98%

“…2) awaits elucidation. For further information concerning sodium overload and NHE-1 in DMD and BMD, the reader should refer to key references (Bkaily et al 1990(Bkaily et al , 2015(Bkaily et al , 2017Al-Khoury et al 2006;Chahine et al 2005;Jacques et al 1997Jacques et al , 2003Honoré et al 2008). …”

Section: Introductionmentioning

confidence: 99%

Na⁺–H⁺exchanger and proton channel in heart failure associated with Becker and Duchenne muscular dystrophies

Bkaily

Jacques

2017

Can. J. Physiol. Pharmacol.

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Cardiomyopathy is found in patients with Duchenne (DMD) and Becker (BMD) muscular dystrophies, which are linked muscle diseases caused by mutations in the dystrophin gene. Dystrophin defects are not limited to DMD but are also present in mild BMD. The hereditary cardiomyopathic hamster of the UM-X7.1 strain is a particular experimental model of heart failure (HF) leading to early death in muscular dystrophy (dystrophin deficiency and sarcoglycan mutation) and heart disease (␦-sarcoglycan deficiency and dystrophin mutation) in human DMD. Using this model, our previous work showed a defect in intracellular sodium homeostasis before the appearance of any apparent biochemical and histological defects. This was attributed to the continual presence of the fetal slow sodium channel, which was also found to be active in human DMD. Due to muscular intracellular acidosis, the intracellular sodium overload in DMD and BMD was also due to sodium influx through the sodium-hydrogen exchanger NHE-1. Lifetime treatment with an NHE-1 inhibitor prevented intracellular Na + overload and early death due to HF. Our previous work also showed that another proton transporter, the voltage-gated proton channel (Hv1), exists in many cell types including heart cells and skeletal muscle fibers. The Hv1 could be indirectly implicated in the beneficial effect of blocking NHE-1.Key words: Becker muscular dystrophy, Duchenne muscular dystrophy, heart failure, NHE-1, proton channel. Résumé :On peut observer une cardiomyopathie chez des patients atteints de dystrophie musculaire de Duchenne (DMD) ou de Becker (DMB). Cette atteinte est liée à des maladies musculaires causées par des mutations dans le gène de la dystrophine. Les défauts dans la dystrophine sont présents dans la DMD, mais dans la DMB légère aussi. Le hamster de la souche UM-X7.1, atteint de cardiomyopathie héréditaire, constitue un modèle expérimental particulier d'insuffisance cardiaque (IC) menant à une mort précoce en cas de dystrophie musculaire (carence en dystrophine et mutation dans le gène de la sarcoglycane) et de maladie cardiaque (carence en ␦-sarcoglycane et mutation dans le gène de la dystrophine) chez des humains atteints de DMD. À l'aide de ce modèle, nos travaux précédents ont montré un défaut dans l'homéostasie du sodium intracellulaire avant l'apparition de tout défaut biochimique ou histologique apparent. Nous avons attribué ce phénomène à la présence continuelle de canaux sodiques lents foetaux, que l'on a aussi retrouvés sous une forme active dans la DMD chez l'humain. En raison de l'acidose intracellulaire musculaire, la surcharge intracellulaire de sodium dans la DMD et la DMB était aussi causée par le passage de sodium par l'échangeur sodium-hydrogène NHE-1. Le traitement à vie avec un inhibiteur du NHE-1 permettait de prévenir la surcharge intracellulaire de Na + et le décès précoce causé par l'IC. Nos travaux précédents ont aussi montré que le Hv1 (canal à protons dépendant du voltage), un autre transporteur de protons, existe dans de nombreux type...

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Protective effect of cerebrocrast on rat brain ischaemia induced by occlusion of both common carotid arteries

Brīede

Дубурс

2006

Cell Biochemistry & Function

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Diabetes mellitus is accompanied by several cardiovascular complications including atherosclerosis, cerebral ischaemia and stroke. We examined the neuroprotective effect of a 1,4-dihydropyridine derivative cerebrocrast (C, a new antidiabetic agent, synthesized in the Latvian Institute of Organic Synthesis) on the level of ATP in the brain, and on changes of the EEG and ECG, as well as blood pressure parameters in anaesthetized Wistar male rats before and during 10-min occlusion of both common carotid arteries. Cerebrocrast was administered i.v. at doses of 1.0 and 10 microg/kg in the v. femoralis 20 min prior to ischaemia. After 10-min ischaemia animals were decapitated and the brain was immediately frozen in liquid nitrogen and subsequently used for analysis of changes of ATP contention. Cerebrocrast, administered at doses of 1.0 and 10 microg/kg 20 min prior to occlusion of both common carotid arteries, completely prevented a fall in the ATP content of brain compared with the control rats. In control rats the content of ATP in brain during ischaemia decreased from 2.77 +/- 0.22 (basal level) to 1.74 +/- 0.20 micromol/g as a result of ischaemia. By administration of cerebrocrast 20 min before occlusion of the arteries, the content of ATP in the brain remained at the level of preischaemia (1.0 microg/kg C + ischaemia 2.82 +/- 0.36; 10 microg/kg C + ischaemia 2.42 +/- 0.22 micromol/g). Analysis of EEG parameters both before and during 10 min of occlusion showed that at a C dose of 1.0 microg/kg before occlusion produced a regular alpha rhythm during ischaemia and prevented cerebral bioelectric activity from significant changes. The depression of basal rhythm was observed at a C dose of 10 microg/kg during ischaemia in two rats out of six as well as an increase in the ECG ST segment above the isoelectric line. Blood pressure was decreased by about 10-20 mm Hg. We propose that pretreatment of rats with cerebrocrast at doses of 1.0 or 10 microg/kg 20 min prior to ischaemia can prevent ischaemic damage of rat brain, maintain necessary energy consumption, promote ATP production in brain cells, and prevent significant changes in EEG and ECG parameters. These properties are important in diabetes mellitus and its evoked cardiovascular complications as stroke, ischaemia, etc.

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Isradipine prevents the development of spontaneously occurring cardiac necrosis in cardiomyopathic hamster

Cited by 7 publications

References 25 publications

Na⁺–H⁺ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Na⁺–H⁺ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Na⁺–H⁺exchanger and proton channel in heart failure associated with Becker and Duchenne muscular dystrophies

Protective effect of cerebrocrast on rat brain ischaemia induced by occlusion of both common carotid arteries

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Isradipine prevents the development of spontaneously occurring cardiac necrosis in cardiomyopathic hamster

Cited by 7 publications

References 25 publications

Na+–H+ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Na+–H+ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Na+–H+exchanger and proton channel in heart failure associated with Becker and Duchenne muscular dystrophies

Protective effect of cerebrocrast on rat brain ischaemia induced by occlusion of both common carotid arteries

Contact Info

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Na⁺–H⁺ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Na⁺–H⁺ exchanger inhibitor prevents early death in hereditary cardiomyopathy

Na⁺–H⁺exchanger and proton channel in heart failure associated with Becker and Duchenne muscular dystrophies