The Effect of Sleep Deprivation on Cardiac Function and Tolerance to Ischemia-Reperfusion Injury in Male Rats

Jeddi, Sajad; Asl, Amir Nezami; Asgari, Alireza; Ghasemi, Asghar

doi:10.5935/abc.20150137

Abstract

Background:

Sleep deprivation (SD) is strongly associated with elevated risk for cardiovascular disease.

Objective:

To determine the effect of SD on basal hemodynamic functions and tolerance to myocardial ischemia-reperfusion (IR) injury in male rats.

Method:

SD was induced by using the flowerpot method for 4 days. Isolated hearts were perfused with Langendorff setup, and the following parameters were measured at baseline and after IR: left ventricular developed pressure (LVDP); heart rate (HR); and the maximum rate of increase and decrease of left ventricular pressure (±dp/dt). Heart NOx level, infarct size and coronary flow CK-MB and LDH were measured after IR. Systolic blood pressure (SBP) was measured at start and end of study.

Results:

In the SD group, the baseline levels of LVDP (19%), +dp/dt (18%), and -dp/dt (21%) were significantly (p < 0.05) lower, and HR (32%) was significantly higher compared to the controls. After ischemia, hearts from SD group displayed a significant increase in HR together with a low hemodynamic function recovery compared to the controls. In the SD group, NOx level in heart, coronary flow CK-MB and LDH and infarct size significantly increased after IR; also SD rats had higher SBP after 4 days.

Conclusion:

Hearts from SD rats had lower basal cardiac function and less tolerance to IR injury, which may be linked to an increase in NO production following IR.

Keywords:
Sleep Deprivation; Sleep Initiation and Maintenance Disorders; Ventricular Dysfunction; Myocardial Ischemia; Myocardial Reperfusion Injury; Nitric Oxide; Rats

Resumo

Fundamento:

A privação de sono (PS) acha-se fortemente associada a alto risco cardiovascular.

Objetivo:

Determinar o efeito da PS nas funções hemodinâmicas basais e tolerância à lesão miocárdica de isquemia‑reperfusão (IR) em ratos machos.

Métodos:

A PS foi induzida com o método da plataforma única por 4 dias. Utilizou-se o modelo de perfusão de coração isolado de Langendorff, medindo-se os seguintes parâmetros nas condições basais e após IR: pressão desenvolvida no ventrículo esquerdo (PDVE), frequência cardíaca (FC) e taxa máxima de aumento e redução da pressão do ventrículo esquerdo (±dp/dt). O nível cardíaco de NOx, o tamanho do infarto e os níveis de CK-MB e LDH no efluente coronário foram medidos após IR. A pressão arterial sistólica (PAS) foi medida no início e no final do estudo.

Resultados:

No grupo PS, os valores basais de PDVE (19%), +dp/dt (18%) e-dp/dt (21%) foram significativamente mais baixos (p < 0,05), e a FC (32%) significativamente mais alta em comparação aos dos controles. Após isquemia, os corações do grupo PS apresentavam um significativo aumento da FC além de uma menor recuperação da função hemodinâmica em comparação aos dos controles. No grupo PS, os níveis de NOx no coração e de CK-MB e LDH no efluente coronário, além do tamanho do infarto, foram significativamente maiores após IR. O grupo PS também apresentou maior PAS após 4 dias.

Conclusão:

Os corações do grupo PS apresentaram menor função cardíaca basal e menor tolerância à lesão de IR, o que pode estar relacionado ao aumento da produção de NO após IR.

Palavras-Chave:
Privação do Sono; Distúrbios do Início e Manutenção do Sono; Disfunção Ventricular; Isquemia Miocárdica; Traumatismo por Reperfusão Miocárdica; Óxido Nítrico; Ratos

Introduction

Cardiac ischemia is the principle cause of human death worldwide¹1 Hausenloy DJ. Signalling pathways in ischaemic postconditioning. Thromb Haemost. 2009;101(4):626-34.^,²2 Ghanbari M, Jeddi S, Bagheripuor F, Ghasemi A. The effect of maternal hypothyroidism on cardiac function and tolerance to ischemia-reperfusion injury in offspring male and female rats. J Endocrinol Invest. 2015;38(8):915-22. and its rate is rising because of co-morbid diseases, such as diabetes and obesity, and also aging.³3 Yin X, Zheng Y, Zhai X, Zhao X, Cai L. Diabetic inhibition of preconditioning- and postconditioning-mediated myocardial protection against ischemia/reperfusion injury. Exp Diabetes Res. 2012;2012:198048. Cardiac ischemia is often induced by the occlusion of coronary arteries and while reperfusion can salvage the ischemic heart from death, it can induce side effects, known as ischemia‑reperfusion (IR) injuries.⁴4 Silvestri P, Di Russo C, Rigattieri S, Fedele S, Todaro D, Ferraiuolo G, et al. MicroRNAs and ischemic heart disease: towards a better comprehension of pathogenesis, new diagnostic tools and new therapeutic targets. Recent Pat Cardiovasc Drug Discov. 2009;4(2):109-18.

Sleep is a vital regulator of cardiovascular function, both in the physiological state and in disease conditions.⁵5 Halperin D. Environmental noise and sleep disturbances: a threat to health? Sleep Science. 2014;7(4):209-12. Previous cohort and case-control studies have indicated that sleep disorders are related to an increased prevalence of cardiovascular disease and even an independent risk factor for the development of that disease.⁶6 Mullington JM, Haack M, Toth M, Serrador JM, Meier-Ewert HK. Cardiovascular, inflammatory, and metabolic consequences of sleep deprivation. Prog Cardiovasc Dis. 2009;51(4):294-302.^,⁷7 Cappuccio FP, Cooper D, D'Elia L, Strazzullo P, Miller MA. Sleep duration predicts cardiovascular outcomes: a systematic review and meta-analysis of prospective studies. Eur Heart J. 2011;32(12):1484-92. Sleep disorders exert harmful effects on a variety of systems with obvious changes in the endocrine, metabolic and immune pathways that are related to unfavorable health outcomes, including diabetes, hypertension, and obesity that are documented to contribute to the development of cardiovascular disease.⁶6 Mullington JM, Haack M, Toth M, Serrador JM, Meier-Ewert HK. Cardiovascular, inflammatory, and metabolic consequences of sleep deprivation. Prog Cardiovasc Dis. 2009;51(4):294-302.^,⁷7 Cappuccio FP, Cooper D, D'Elia L, Strazzullo P, Miller MA. Sleep duration predicts cardiovascular outcomes: a systematic review and meta-analysis of prospective studies. Eur Heart J. 2011;32(12):1484-92.

Nitric oxide (NO) is synthesized by NO synthase enzymes in the heart and plays a vital role in cardiac functions. Despite the evidence highlighting the role of ischemia in a rise in NO production,⁸8 Jeddi S, Zaman J, Ghasemi A. Effects of ischemic postconditioning on the hemodynamic parameters and heart nitric oxide levels of hypothyroid rats. Arq Bras Cardiol. 2015;104(2):136-43.^,⁹9 Zaman J, Jeddi S, Ghasemi A. The effects of ischemic postconditioning on myocardial function and nitric oxide metabolites following ischemia-reperfusion in hyperthyroid rats. Korean J Physiol Pharmacol. 2014;18(6):481-7. no studies have yet examined the changes in the NO content in the hearts of sleep deprivation (SD) rats and its contribution to IR injury. Moreover, to the best of our knowledge, there is no study addressing the effects of SD on basal cardiac function and cardiac tolerance following IR injury. Therefore, the aim of this study was to determine the effect of SD on basal hemodynamic functions and tolerance to myocardial IR injury in male rats. In addition, changes in NO metabolites (NOx) following IR injury were also assessed.

Methods

Animals

In this study, 16 male Wistar rats (2-month old) were obtained from laboratory animal house of the Research Institute for Endocrine Sciences (RIES), Shahid Beheshti University of Medical Sciences. All animals were housed in an animal room with temperature and light controlled conditions (22 ± 2ºC 12/12-h dark-light cycle), and had free access to food and water at all times.

The proposal of this study was approved by the Institutional Animal Care and Use Committee (IACUC) of the RIES (Permit Number: 12 EC RIES 93/11/27), Shahid Beheshti University of Medical Sciences (Tehran, Iran).

Induction of REM sleep deprivation

Male rats were deprived of rapid-eye-movement (REM) sleep for 96 hours. Rapid-eye-movement SD was induced by using the flowerpot technique.¹⁰10 Arthaud S, Varin C, Gay N, Libourel P, Chauveau F, Fort P, et al. Paradoxical (REM) sleep deprivation in mice using the small-platforms-over-water method: polysomnographic analyses and melanin-concentrating hormone and hypocretin/orexin neuronal activation before, during and after deprivation. J Sleep Res. 2015;24(3):309-19. Briefly, rats were placed on an inverted pot (platform of 7-cm diameter) surrounded by water reaching to a level of 1cm under the bottom of the pot. Tank's water was refreshed every morning. Prior to depriving rats of sleep, they were trained for 1-2 hours to stay steady on the platform and not to fall into the water. After training, on the day of experiment, they were taken from their home cage and placed individually in the water tank.

For experiments, animals were randomly divided into 2 groups (n = 8 each): Control and SD.

Isolated heart preparation

All animals were anesthetized with an intraperitoneal injection of ketamine and xylazine (50 mg/kg and 10 mg/kg, respectively). Once fully anesthetized, the thorax was opened and the hearts of control and SD rats were rapidly excised and embedded in an ice-cold perfusion buffer. The aortas were then cannulated and the whole preparation mounted in the Langendorff perfusion apparatus and perfused through the aorta with a Krebs-Henseleit solution containing (mM/L): NaCl 118, NaHCO₃ 25, KCl 4.7, MgCl₂ 1.2, CaCl₂ 2.5, KH₂PO₄ 1.2, and glucose 11 at a constant pressure (75 mm Hg) and pH of 7.4. The Krebs solution was gassed with a combination of 95% O₂ and 5% CO₂ at 37ºC. All isolated hearts were stabilized for 20 minutes with the purpose of obtaining baseline data. After stabilization, hearts were subjected to global ischemia for 30 minutes followed by reperfusion for 45 minutes. Left ventricular hemodynamic parameters were measured via a latex balloon inserted in the left ventricle. The balloon capacity was adjusted to create 5-10 mm Hg of end-diastolic pressure in all hearts by filling it with water. Hemodynamic parameters [left ventricular end-diastolic pressure (LVEDP), heart rate (HR), left ventricular developed pressure (LVDP), and the maximum rate of increase and decrease of left ventricular pressure (±dp/dt)] were digitized and recorded by a data acquisition system (Power Lab, AD Instrument, Australia).

Measurement of NOx

Following 45-min reperfusion, samples of left ventricular tissue were immediately frozen in liquid nitrogen and stored at -80ºC. NOx contents in heart homogenates were determined using the Griess method¹¹11 Ghasemi A, Zahediasl S. Preanalytical and analytical considerations for measuring nitric oxide metabolites in serum or plasma using the Griess method. Clin Lab. 2012;58(7-8):615-24.. Briefly, after homogenization of samples in phosphate-buffered saline (1:5, w/v), the homogenates were centrifuged at 15,000 g for 20 min at 4ºC. The supernatants were removed from the homogenates and were deproteinized by addition of zinc sulfate (15 mg/mL). Tissue samples, 100 μL of the supernatant were added to a microplate well, and 100 μL vanadium (III) chloride (8 mg/mL) were added to each well (for reduction of nitrate to nitrite), followed by addition of 50 μL sulfanilamide (2%) and 50 μL NEDD (N-(1-naphtyl) ethylendiamine dihydrochloride) (0.1%). After 30-min incubation at 37ºC, the absorbance was read at 540 nm using the ELISA reader (BioTek, Powerwave XS2). NOx concentrations in heart homogenate samples were measured from the linear standard curve established by 0-100 μmol/L of sodium nitrate. Heart NOx levels are presented as μmol/L. Intra-assay coefficient of variation was 4.9%.

Measurement of infarct size

At the end of the reperfusion period, infarct sizes were determined as described previously. The frozen heart samples were cut into thin slices (2-3 mm) and were incubated for 10 minutes in 1% of 2,3,5-triphenyltetrazolium chloride in phosphate buffer solution 20 mM/L, pH 7.4 at 37ºC. The slices were immersed in 10% formalin for 24 hours to identify viable myocardium as red stained, easily discriminable from unstained necrotic tissue. The sections were then photographed using a digital camera (Samsung, Japan, version DV101). The infarct size was measured by Photoshop CS6 software (version 13) and expressed as percentage of the total area.²2 Ghanbari M, Jeddi S, Bagheripuor F, Ghasemi A. The effect of maternal hypothyroidism on cardiac function and tolerance to ischemia-reperfusion injury in offspring male and female rats. J Endocrinol Invest. 2015;38(8):915-22.

Measurement of creatine kinase (CK) and lactate dehydrogenase (LDH)

Samples of coronary flow were collected for 5 minutes after start of reperfusion for measuring the myocardial enzyme leakage, CK-MB and LDH.¹²12 Amani M, Jeddi S, Ahmadiasl N, Usefzade N, Zaman J. Effect of HEMADO on level of CK-MB and LDH enzymes after ischemia/reperfusion injury in isolated rat heart. Bioimpacts. 2013;3(2):101-4. The CK-MB and LDH levels in the coronary effluent were determined by spectrophotometric method via CK-MB kit and LDH kit (Pars Azmoon, Iran) and the results were expressed as U/L.

Statistical analysis

All values are expressed as means ± SEM. Statistical analysis was performed using SPSS software (SPSS, Chicago, IL, USA; version 20). The Shapiro-Wilk test was used to check the normality of study data, and then parametric or non-parametric tests were used to analyze normal or non‑normal data distribution, respectively.¹³13 Ghasemi A, Zahediasl S. Normality tests for statistical analysis: a guide for non-statisticians. Int J Endocrinol Metab. 2012;10(2):486-9. Therefore, repeated measurement analysis of variance (ANOVA) was used to compare hemodynamic parameters (LVDP, LVEDP, ±dp/dt, and HR) in different times. The Student t test was used to compare blood pressure, infarct size, heart NOx levels and coronary flow CK-MB and LDH between control and SD groups. Two-sided p-values < 0.05 were considered statistically significant.

Results

After 96 hours of SD, the rats showed a significant increase in systolic blood pressure (SBP) compared to the control group (Figure 1).

Figure 1
Comparison of changes in systolic blood pressure in control and sleep deprivation groups. Values shown as mean ± SEM.

Effects of SD on hemodynamic parameters in isolated heart during the stabilization and IR periods are shown in Table 1, Figure 2, and Figure 3. As seen, during the stabilization period, hearts from SD rats had significantly lower baseline LVDP and ±dp/dt, and higher HR (p < 0.05) compared to the control group (Table 1). When there was ischemia, the LVDP, ±dp/dt, and HR rapidly decreased and stopped in the isolated hearts. In both groups, LVEDP was gradually increased during the 30 minutes of ischemia, however the SDgroup displayed a significant increase (p < 0.05) compared to the control group (Figure 2). Compared with the control group, post-ischemic LVDP and ±dp/dt were significantly lower and HR was higher in the SD group (p < 0.05) (Figure 3-A, B, C, and D).

Thumbnail

Table 1
Cardiac function at the stabilization period (baseline data)

Figure 2
Change in left ventricular end-diastolic pressure (LVEDP) (ischemic contracture) during experiment. Values shown as mean ± SEM (n = 8 rats)

Figure 3
Recovery of cardiac function after ischemia-reperfusion injury. A. Left ventricular developed pressure (LVDP); B. Heart rate; C. Peak rates of positive changes in left ventricular pressure (+dp/dt); D. Peak rates of negative changes in left ventricular pressure (- dp/dt). Values shown as mean ± SEM (n = 8 rats)

IR induced a marked increase in the heart NOx level in the SD group compared with the control group (Figure 4).

Figure 4
Change in NOx in control and sleep deprivation groups in heart after ischemia. Values shown as mean ± SEM (n = 8 rats)

Coronary flow CK-MB and LDH levels were significantly (p < 0.05) higher in the SD group compared to the control group (p < 0.05) (Figure 5).

Figure 5
Change in coronary flow CK-MB (A) and LDH (B) in control and sleep deprivation groups in start of reperfusion. Values shown as mean ± SEM (n = 8 rats)

Sleep deprivation significantly increased the infarct size in SD rats compared to control rats (Figure 6).

Figure 6
The alterations of infarct size in heart of control and sleep deprivation rats. Values shown as mean ± SEM (n = 8 rats)

Discussion

The results of this study showed for the first time that SD for 96 hours induces negative inotropic and chronotropic effects on the hearts isolated from male rats and increases the IR-induced injury in those hearts, which may be linked to increasing the NO production after IR.

In this study, SBP was higher in the SD group compared to controls. Several studies have found that experimental SD leads to increased blood pressure, which is in line with our findings. Neves et al¹⁴14 Neves FA, Marson O, Baumgratz RP, Bossolan D, Ginosa M, Ribeiro AB, et al. Rapid eye movement sleep deprivation and hypertension: genetic influence. Hypertension. 1992;19(2 Suppl):II202-6. have shown that rats with 72-hour REM SD had higher blood pressure compared with controls. Joukar et al¹⁵15 Joukar S, Ghorbani-Shahrbabaki S, Hajali V, Sheibani V, Naghsh N. Susceptibility to life-threatening ventricular arrhythmias in an animal model of paradoxical sleep deprivation. Sleep Med. 2013;14(12):1277-82. have indicated that SD resulted in a significant increase in blood pressure in rats by using the similar method. De Mesquita and Hale¹⁶16 DeMesquita S, Hale GA. Cardiopulmonary regulation after rapid-eye-movement sleep deprivation. J Appl Physiol (1985). 1992;72:970-6. have also shown that SD in rats led to increasing blood pressure following 114 hours of REM SD. As stated by others, blood pressure could have increased during SD due to either increased sympathetic outflow to the heart or periphery, or changes in baroreflex sensitivity to a higher level, or a combination of both.⁶6 Mullington JM, Haack M, Toth M, Serrador JM, Meier-Ewert HK. Cardiovascular, inflammatory, and metabolic consequences of sleep deprivation. Prog Cardiovasc Dis. 2009;51(4):294-302.^,¹⁷17 Kato M, Phillips BG, Sigurdsson G, Narkiewicz K, Pesek CA, Somers VK. Effects of sleep deprivation on neural circulatory control. Hypertension. 2000;35(5):1173-5.^,¹⁸18 Ogawa Y, Kanbayashi T, Saito Y, Takahashi Y, Kitajima T, Takahashi K, et al. Total sleep deprivation elevates blood pressure through arterial baroreflex resetting: a study with microneurographic technique. Sleep. 2003;26(8):986-9.

Pre-ischemic and reperfusion HR were higher in the SD group than in controls, which is consistent with the reports by others. Sgoifo et al,¹⁹19 Sgoifo A, Buwalda B, Roos M, Costoli T, Merati G, Meerlo P. Effects of sleep deprivation on cardiac autonomic and pituitary-adrenocortical stress reactivity in rats. Psychoneuroendocrinology. 2006;31(2):197-208. Carvalho et al,²⁰20 Carvalho RS, Perry JC, Campos RR, Andersen ML, Tufik S, Bergamaschi CT. Paradoxical sleep deprivation increases mortality in myocardial infarcted rats. Sleep and Biol Rhythms. 2014;12(3):216-9. and Almeida et al²¹21 Almeida FR, Perry JC, Futuro-Neto HA, Almeida VR, Sebastião RM, Andersen ML, et al. Cardiovascular function alterations induced by acute paradoxical sleep deprivation in rats. Clin Exp Hypertens. 2014;36(8):567-71. have reported that SD rats exhibited an increased HR and were vulnerable to ventricular arrhythmias. The mechanism of action of SD on HR during perfusion and reperfusion is not completely understood. In this regard, studies have shown that SD increases HR through various mechanisms. One possible cause for the significant increase in HR in SD rats before and after ischemia may have resulted from the immobility stress induced by the flowerpot technique. Sleep deprivation affects the basal activity of the stress system by increasing the corticosterone and adrenocorticotropic hormone concentrations and the subsequent response to an acute suppression in the cardiac autonomic and hypothalamic-pituitary-adrenal axis.¹⁹19 Sgoifo A, Buwalda B, Roos M, Costoli T, Merati G, Meerlo P. Effects of sleep deprivation on cardiac autonomic and pituitary-adrenocortical stress reactivity in rats. Psychoneuroendocrinology. 2006;31(2):197-208.^,²²22 Andersen ML, Martins PJ, D'Almeida V, Bignotto M, Tufik S. Endocrinological and catecholaminergic alterations during sleep deprivation and recovery in male rats. J Sleep Res. 2005;14(1):83-90.

We recorded lower baseline LVDP and ± dp/dt in the SD group, which indicate that SD could affect the normal heart function. The exact mechanisms of the SD effects on baseline cardiac functions are not fully understood and need further elucidation, but SD has been suggested to indirectly increase cardiovascular disease by increasing inflammation and cortisol secretion, altering growth hormone metabolism and changing the circulating levels of ghrelin and leptin.⁷7 Cappuccio FP, Cooper D, D'Elia L, Strazzullo P, Miller MA. Sleep duration predicts cardiovascular outcomes: a systematic review and meta-analysis of prospective studies. Eur Heart J. 2011;32(12):1484-92. In addition, we showed for the first time that, after ischemia, hearts from the SD group displayed a significantly low hemodynamic function recovery compared to controls, indicating that these hearts are susceptible to the IR injury, as confirmed by the increase in the LDH and CK-MB levels in the coronary effluent and the rise in the infarct size.

In this study, consistent with other studies on disease states, such as hyperthyroidism,⁹9 Zaman J, Jeddi S, Ghasemi A. The effects of ischemic postconditioning on myocardial function and nitric oxide metabolites following ischemia-reperfusion in hyperthyroid rats. Korean J Physiol Pharmacol. 2014;18(6):481-7. diabetes²³23 Badalzadeh R, Mohammadi M, Najafi M, Ahmadiasl N, Farajnia S, Ebrahimi H. The additive effects of ischemic postconditioning and cyclosporine-A on nitric oxide activity and functions of diabetic myocardium injured by ischemia/reperfusion. J Cardiovasc Pharmacol Ther. 2012;17(2):181-9. and maternal hypothyroidism,²2 Ghanbari M, Jeddi S, Bagheripuor F, Ghasemi A. The effect of maternal hypothyroidism on cardiac function and tolerance to ischemia-reperfusion injury in offspring male and female rats. J Endocrinol Invest. 2015;38(8):915-22. ischemia increased the CK-MB and LDH levels and the infarct size in the SD group, which showed heart cell necrosis. The heart cells contracted during long or severe ischemia and start of reperfusion, causing mechanical stiffness and tissue necrosis. Contracted cells put pressure on neighboring cells and cause their decomposition and development of contraction, leading to widespread necrosis.¹²12 Amani M, Jeddi S, Ahmadiasl N, Usefzade N, Zaman J. Effect of HEMADO on level of CK-MB and LDH enzymes after ischemia/reperfusion injury in isolated rat heart. Bioimpacts. 2013;3(2):101-4.^,²⁴24 Moens AL, Claeys MJ, Timmermans JP, Vrints CJ. Myocardial ischemia/reperfusion-injury, a clinical view on a complex pathophysiological process. Int J Cardiol. 2005;100(2):179-90.

In this study, the capacity of the balloon in the left ventricle was fixed during ischemia and reperfusion, so the increase in LVEDP resulted from stiffness in the left ventricular wall or ventricular contracture. Thus, SD could be said to increase contracture and accordingly to significantly increase the subsequent necrosis in the IR period in the heart of SD rats. Increasing Ca²⁺ concentration in heart cells and ATP depletion have been reported to be important factors in ischemic contracture.²⁵25 Segal J, Masalha S, Schwalb H, Merin G, Borman JB, Uretzky G. Acute effect of thyroid hormone in the rat heart: role of calcium. J Endocrinol. 1996;149(1):73-80.

The function of NO in the cardiovascular system after ischemia has not been fully enlightened. A few studies have considered a negative role for NO in myocardial IR injury, whereas others have reported a protecting role. Recent studies have shown that the NO level of myocardial cells is in a low range at baseline and increases during IR injury. While a low range increase in NO production may be cardioprotective, a vast increase appears to be injurious. At high levels, NO reacts with superoxide and produces peroxynitrite, which is a highly toxic agent that could induce apoptosis in heart cells.⁸8 Jeddi S, Zaman J, Ghasemi A. Effects of ischemic postconditioning on the hemodynamic parameters and heart nitric oxide levels of hypothyroid rats. Arq Bras Cardiol. 2015;104(2):136-43.^,⁹9 Zaman J, Jeddi S, Ghasemi A. The effects of ischemic postconditioning on myocardial function and nitric oxide metabolites following ischemia-reperfusion in hyperthyroid rats. Korean J Physiol Pharmacol. 2014;18(6):481-7. Our results show that SD increases IR-induced injuries in rat hearts, which may possibly be linked to elevated NO levels after ischemia. Thus, it could be hypothesized that SD may lead to reperfusion injury by increasing the NO production.

Regarding the limitations of this study, we used global ischemia, which has been commonly used in the Langendorff-perfused heart model. However, the use of the regional ischemia model has been reported to be clinically more relevant.²⁶26 Zaman J, Jeddi S, Daneshpour MS, Zarkesh M, Daneshian Z, Ghasemi A. Ischemic postconditioning provides cardioprotective and antiapoptotic effects against ischemia-reperfusion injury through iNOS inhibition in hyperthyroid rats. Gene. 2015;570(2):185-90. In addition, our results are limited to male rats, while SD affects cardiac functions in both sexes.²⁷27 Ferrara M, Bottasso A, Tempesta D, Carrieri M, De Gennaro L, Ponti G. Gender differences in sleep deprivation effects on risk and inequality aversion: evidence from an economic experiment. PLoS One. 2015;10(3):e0120029.

Conclusion

Based on our findings we conclude that the hearts of SD rats had lower basal cardiac function and less tolerance to the IR injury, confirmed by the increase in LDH and CK-MB levels in coronary flow. In addition, the rise in the infarct size may be due to an increase in the NO production after IR.

Sources of Funding

There were no external funding sources for this study.
Study Association

This study is not associated with any thesis or dissertation work.

Acknowledgments

The authors thank Ms. N. Shiva for the critical editing of English grammar and syntax of the manuscript.

References

¹
Hausenloy DJ. Signalling pathways in ischaemic postconditioning. Thromb Haemost. 2009;101(4):626-34.
²
Ghanbari M, Jeddi S, Bagheripuor F, Ghasemi A. The effect of maternal hypothyroidism on cardiac function and tolerance to ischemia-reperfusion injury in offspring male and female rats. J Endocrinol Invest. 2015;38(8):915-22.
³
Yin X, Zheng Y, Zhai X, Zhao X, Cai L. Diabetic inhibition of preconditioning- and postconditioning-mediated myocardial protection against ischemia/reperfusion injury. Exp Diabetes Res. 2012;2012:198048.
⁴
Silvestri P, Di Russo C, Rigattieri S, Fedele S, Todaro D, Ferraiuolo G, et al. MicroRNAs and ischemic heart disease: towards a better comprehension of pathogenesis, new diagnostic tools and new therapeutic targets. Recent Pat Cardiovasc Drug Discov. 2009;4(2):109-18.
⁵
Halperin D. Environmental noise and sleep disturbances: a threat to health? Sleep Science. 2014;7(4):209-12.
⁶
Mullington JM, Haack M, Toth M, Serrador JM, Meier-Ewert HK. Cardiovascular, inflammatory, and metabolic consequences of sleep deprivation. Prog Cardiovasc Dis. 2009;51(4):294-302.
⁷
Cappuccio FP, Cooper D, D'Elia L, Strazzullo P, Miller MA. Sleep duration predicts cardiovascular outcomes: a systematic review and meta-analysis of prospective studies. Eur Heart J. 2011;32(12):1484-92.
⁸
Jeddi S, Zaman J, Ghasemi A. Effects of ischemic postconditioning on the hemodynamic parameters and heart nitric oxide levels of hypothyroid rats. Arq Bras Cardiol. 2015;104(2):136-43.
⁹
Zaman J, Jeddi S, Ghasemi A. The effects of ischemic postconditioning on myocardial function and nitric oxide metabolites following ischemia-reperfusion in hyperthyroid rats. Korean J Physiol Pharmacol. 2014;18(6):481-7.
¹⁰
Arthaud S, Varin C, Gay N, Libourel P, Chauveau F, Fort P, et al. Paradoxical (REM) sleep deprivation in mice using the small-platforms-over-water method: polysomnographic analyses and melanin-concentrating hormone and hypocretin/orexin neuronal activation before, during and after deprivation. J Sleep Res. 2015;24(3):309-19.
¹¹
Ghasemi A, Zahediasl S. Preanalytical and analytical considerations for measuring nitric oxide metabolites in serum or plasma using the Griess method. Clin Lab. 2012;58(7-8):615-24.
¹²
Amani M, Jeddi S, Ahmadiasl N, Usefzade N, Zaman J. Effect of HEMADO on level of CK-MB and LDH enzymes after ischemia/reperfusion injury in isolated rat heart. Bioimpacts. 2013;3(2):101-4.
¹³
Ghasemi A, Zahediasl S. Normality tests for statistical analysis: a guide for non-statisticians. Int J Endocrinol Metab. 2012;10(2):486-9.
¹⁴
Neves FA, Marson O, Baumgratz RP, Bossolan D, Ginosa M, Ribeiro AB, et al. Rapid eye movement sleep deprivation and hypertension: genetic influence. Hypertension. 1992;19(2 Suppl):II202-6.
¹⁵
Joukar S, Ghorbani-Shahrbabaki S, Hajali V, Sheibani V, Naghsh N. Susceptibility to life-threatening ventricular arrhythmias in an animal model of paradoxical sleep deprivation. Sleep Med. 2013;14(12):1277-82.
¹⁶
DeMesquita S, Hale GA. Cardiopulmonary regulation after rapid-eye-movement sleep deprivation. J Appl Physiol (1985). 1992;72:970-6.
¹⁷
Kato M, Phillips BG, Sigurdsson G, Narkiewicz K, Pesek CA, Somers VK. Effects of sleep deprivation on neural circulatory control. Hypertension. 2000;35(5):1173-5.
¹⁸
Ogawa Y, Kanbayashi T, Saito Y, Takahashi Y, Kitajima T, Takahashi K, et al. Total sleep deprivation elevates blood pressure through arterial baroreflex resetting: a study with microneurographic technique. Sleep. 2003;26(8):986-9.
¹⁹
Sgoifo A, Buwalda B, Roos M, Costoli T, Merati G, Meerlo P. Effects of sleep deprivation on cardiac autonomic and pituitary-adrenocortical stress reactivity in rats. Psychoneuroendocrinology. 2006;31(2):197-208.
²⁰
Carvalho RS, Perry JC, Campos RR, Andersen ML, Tufik S, Bergamaschi CT. Paradoxical sleep deprivation increases mortality in myocardial infarcted rats. Sleep and Biol Rhythms. 2014;12(3):216-9.
²¹
Almeida FR, Perry JC, Futuro-Neto HA, Almeida VR, Sebastião RM, Andersen ML, et al. Cardiovascular function alterations induced by acute paradoxical sleep deprivation in rats. Clin Exp Hypertens. 2014;36(8):567-71.
²²
Andersen ML, Martins PJ, D'Almeida V, Bignotto M, Tufik S. Endocrinological and catecholaminergic alterations during sleep deprivation and recovery in male rats. J Sleep Res. 2005;14(1):83-90.
²³
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Publication Dates

Publication in this collection
10 Nov 2015
Date of issue
Jan 2016

History

Received
24 June 2015
Accepted
06 Aug 2015

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] Sources of Funding

There were no external funding sources for this study.

[2] Study Association

This study is not associated with any thesis or dissertation work.

	Control	Sleep deprivation	p value
LVDP^* * p < 0.05.	93.14 ± 4.9	75.5 ± 3.5	0.035
Heart rate^* * p < 0.05.	262.2 ± 11.1	347.5 ± 19.7	0.003
dp.dt max^* * p < 0.05.	2897.1 ± 75.1	2367 ± 222.7	0.021
dp.dt min^* * p < 0.05.	2555.3 ± 227.6	1788.8 ± 105.9	0.046

Brasil