Altered Myocardial Function and Metabolism in Chronic Diabetes Mellitus without Ischemia in Dogs

Regan, Timothy J.; Ettinger, Philip O.; Khan, Mohammad Ibrahim; Jesrani, Mohan U.; Lyons, Michael M.; Oldewurtel, Henry A.; Weber, Marilyn A.

doi:10.1161/01.res.35.2.222

Cited by 282 publications

(109 citation statements)

References 48 publications

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“…This diminution of EDP can be taken as an indicator of an improved relaxation of the diabetic heart. Since the velocity of relaxation delayed in diabetes was not influenced by captopril and since the diabetes-induced increase in EDP largely reflects the increased stiffness of ventricles in diabetes by accumulation of collagen and other matrix proteins [4,9,19,25], we assume that the diminution of the end diastolic pressure reflects changes in the texture of cardiac vasculature and wall, but not an effect of the ACE inhibitor on the electric properties of the heart. In line with this assumption it has been shown that ACE inhibitors inhibit the deposition of collagen and other matrix proteins and thus can prevent the development of interstitial fibrosis [25].…”

Section: Discussionmentioning

confidence: 99%

“…Additionally or alternatively, our results could be explained by a delayed degradation of bradykinin. Bradykinin has been shown to increase the nutritional flow and the permeability of coronary vasculature leading to an improved local myocardial perfusion [17,19,30]. Furthermore, it has been shown that ACE inhibition and delayed degradation of bradykinin can prevent endothelial dysfunction induced by a variety of pathophysiological states [27,48].…”

Section: Discussionmentioning

confidence: 99%

“…Microangiopathic changes [14][15][16], abnormalities in vascular reactivity [15,17], altered autonomic function [9,18], increased stiffness of the ventricular wall and perivascular thickening, interstitial accumulation of connective tissue and matrix proteins [4,9,18,19], and defects in the regulation of calcium homeostasis [20] have been claimed to contribute as aetiological factors to disturbances of heart function in diabetes.…”

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confidence: 99%

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The ACE-inhibitor captopril improves myocardial perfusion in spontaneously diabetic (BB) rats

1995

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SummaryThe aim of this study was to examine the influence of inhibition on angiotensin converting enzyme (ACE) of myocardial function and perfusion of the rat impaired by diabetes. Spontaneously diabetic rats were treated with the ACE-inhibitor captopril for 4 months. Cardiac performance was analysed in the isolated heart perfused at constant volume. Epicardial perfusion was determined by measuring changes in epicardial fluorescence after injection of a bolus of fluoresceinisothiocyanate-dextrane (3 kDa) as described previously. As compared to untreated diabetic controls, captopril prevented the increase of end diastolic pressure, coronary perfusion pressure and vascular resistance. The intravascular volume was enlarged and the epicardial perfusion rate increased in hearts of diabetic rats treated with captopril as compared to diabetic controls. Treatment of diabetic rats with the ACE-inhibitor captopril (1) increases the number of perfused capillaries, and (2) can partly prevent the development of cardiac dysfunction in diabetes. Together with morphological data demonstrating an inhibition of interstitial and perivascular fibrosis in hearts of diabetic rats treated with captopril, our data suggest that ACE-inhibition is cardioprotective in diabetes. These observations are also compatible with the assumption that an accelerated generation of angiotensin II may be involved in the pathophysiological chain of events leading to diabetic cardiopathy. [Diabetologia (1995) 38: 509-517] Key words Diabetes mellitus, cardiopathy, ACE-inhibition, captopril, BB rats, regional perfusion, myocardial function.The incidence of cardiovascular complications is severely increased in diabetes mellitus by the development of macrovascular complications. However, coronary heart disease can only partly explain the increased rate of cardiovascular complications in diabetes, since cardiac risk remains elevated even in the absence of atherosclerosis [1][2][3]. In patients, impairment of diastolic relaxation and signs of cardiac neu- ropathy have been consistently reported [3,4]. Additionally, cardiac performance is further impaired in diabetic patients by development of small vessel disease [5,6]. In animal models using chemically-induced forms of insulin deficiency or spontaneously diabetic rats and mice, the metabolic disturbances following insulin deficiency cause impairment of diastolic and systolic heart performance, which can be totally prevented by treatment of the animals with insulin [7][8][9][10][11]. The various forms of cardiac dysfunction in diabetes which develop independently from coronary heart disease, are often called "diabetic cardiomyopathy" [12][13][14].The mechanisms underlying these complex disturbances of heart function in diabetes are not fully understood and several hypotheses have been suggested to link the metabolic disturbances observed in the diabetic heart with impairment of heart function [4,

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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The ACE-inhibitor captopril improves myocardial perfusion in spontaneously diabetic (BB) rats

1995

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“…2 " 4 Decreased cardiac contractility in diabetic animals seems quite well established. 5 ' 6 The pathophysiologic mechanisms that underlie the decreased contractility are currently unclear. In particular, it is unknown if changes in the state of contractile proteins contribute to the decreased contractility of the diabetic heart.…”

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confidence: 99%

Diabetes Mellitus Induces Changes in Cardiac Myosin of the Rat

Dillmann

1980

Diabetes

280

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SUMMARYDecreased contractility has been reported in the diabetic heart. Because a close correlation exists between contractility and the activity of Ca 2+ ATPase of purified actinomyosin and myosin, Ca 2+ ATPase activity was determined in control and diabetic rats. In control rats, actinomyosin ATPase was 0.59 ± 0.05 /xmol Pi/mg protein/min and had decreased by 35% to 0.38 ± 0.04 in diabetic rats (P < 0.025). Myosin ATPase activity was 1.25 ± 0.09 /xmol Pi/mg protein/min in control rats and had decreased by 45% to 0.67 ± 0.05 in diabetic animals (P < 0.01). To investigate the decrease in myosin ATPase activity further, ventricular myosin was separated by pyrophosphate polyacrylamide electrophoresis into its three authentic components, V,, V 2 , and V 3 myosin. V 1 has the highest mobility and Ca 2 ATPase activity (1.27 ± 0.3 arbitrary units) and represents 72% of control myosin, whereas V 3 has the lowest mobility and Ca 2+ ATPase activity (0.16 ± 0.08 units) and constitutes 13% of myosin. A marked change in the predominance of V, and V 3 myosin components occurs in diabetic rats where V 3 myosin predominates, representing 68% of total myosin with V 1 myosin constituting only 15%. Ca 2+ ATPase activities of V,, V 2 , and V 3 myosin in control and diabetic hearts are similar; however, the predominance of V 3 myosin in diabetic rats can account for the decreased Ca 2+ ATPase activity of diabetic myosin. The diabetes-induced changes in myosin ATPase activity and myosin isoenzyme distribution can be reverted to control levels by insulin administration. Decreased cardiac contractility in diabetic animals seems quite well established. 5 ' 6 The pathophysiologic mechanisms that underlie the decreased contractility are currently unclear. In particular, it is unknown if changes in the state of contractile proteins contribute to the decreased contractility of the diabetic heart. The activity of Ca 2+ -activated ATPase of actinomyosin and myosin has not been determined in diabetic hearts. A close correlation between the activity of Ca 2+ -activated ATPase of actinomyosin or myosin and cardiac contractility has been well established.7 Furthermore, recent reports have described the occurrence of cardiac myosin isoenzymes.8 -10 These myosin isoenzymes can be separated by electrophoretic techniques into three components that differ in Ca 2+ ATPase activity.The following studies were undertaken to assess the activity of Ca 2+ATPase of actinomyosin and myosin arid to determine if changes in the distribution of myosin isoenzymes occur in diabetic rat hearts. MATERIALS AND METHODSMale Sprague-Dawley rats between 6 and 8 wk of age were used for all experiments. Control and diabetic animals were age-and litter-matched. Rats were made diabetic by i.v. administration of 65 mg streptozotoc in/kg body wt and maintained in a diabetic state for 4 wk. After being diabetic for 4 wk, rats were injected s.c. with 2 U protamine zinc insulin (PSI)/day for 4 wk.11 To assure that animals were diabetic, blood sugars were determined 4 days and 4 wk...

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“…Já Rubler et al (1972), Arduino (1973), Regan et al (1974), Kannel & Mcgee (1979), Koltai et al (1984), Chen (2000), Bell (2003) e Gilles (2003) são autores que descreveram a etiologia, a patologia e a sintomatologia do Diabetes mellitus, que foi a doença de estudo deste trabalho. Goodfellow (1997), Neckar et al (2001), referem-se ao acú-mulo de colágeno em corações diabéticos ser o principal fator pela alteração funcional do miocárdio.…”

Section: Discussão E Conclusõesunclassified

Morfometria das fibras colágeno cardíaco em ratos sadios e diabéticos suplementados com vitamina C

et al. 2011

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O aumento do conteúdo de fibras colágenas no coração de diabéticos é um fato bastante conhecido, suas conseqüências ainda são objeto de estudo e causam certa controvérsia, portanto este trabalho objetivou estudar a variação na quantidade das fibras de colágeno cardíacas em animais normais e diabéticos tratados pela vitamina C. Para isso foram selecionados 32 ratos Wistar, 16 diabéticos induzidos pela injeção endovenosa de estreptozootocina e 16 normais, sendo metade deles tratados com Vitamina C (diabéticos e normais) por um período de 90 dias. Após período experimental, os corações foram retirados e processados segundo protocolo convencional para microscopia óptica e coloração específica para colágeno. Os resultados mostram que animais diabéticos apresentam maior quantidade de fibras de colágeno cardíacas e que o tratamento com a vitamina C determinou um menor acúmulo na quantidade dessas fibras.

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Altered Myocardial Function and Metabolism in Chronic Diabetes Mellitus without Ischemia in Dogs

Cited by 282 publications

References 48 publications

The ACE-inhibitor captopril improves myocardial perfusion in spontaneously diabetic (BB) rats

The ACE-inhibitor captopril improves myocardial perfusion in spontaneously diabetic (BB) rats

Diabetes Mellitus Induces Changes in Cardiac Myosin of the Rat

Morfometria das fibras colágeno cardíaco em ratos sadios e diabéticos suplementados com vitamina C

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