Leptin’s regulation of obesity-induced cardiac extracellular matrix remodeling

Zibadi, Sherma; Cordova, Felina M.; Slack, Elise; Watson, Ronald R.; Larson, Douglas F.

doi:10.1007/s12012-011-9124-0

Cited by 54 publications

(48 citation statements)

References 32 publications

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“…19 In particular, the metabolic effects of obesity resulting in dyslipidemia and insulin resistance seem to be the most likely mediators of changes in maternal cardiac function through changes in the composition and material properties of the myocardium. [19][20][21][22][23][24] This assertion is indirectly supported by a recent study demonstrating that Ϸ20% of women who previously had a normotensive FGR pregnancy had features of metabolic syndrome. 25 The endothelial dysfunction is another known mechanism of diastolic impairment 26 and could also play a role in the diastolic abnormalities seen in normotensive FGR, as well as PE pregnancies.…”

Section: Melchiorre Et Al Maternal Cardiac Function In Fgr Pregnanciesmentioning

confidence: 81%

Maternal Cardiovascular Impairment in Pregnancies Complicated by Severe Fetal Growth Restriction

et al. 2012

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Abstract-Fetal growth restriction and preeclampsia are both conditions of placental etiology and associated to increased risk for the long-term development of cardiovascular disease in the mother. At presentation, preeclampsia is associated with maternal global diastolic dysfunction, which is determined, at least in part, by increased afterload and myocardial stiffness. The aim of this study is to test the hypothesis that women with normotensive fetal growth-restricted pregnancies also exhibit global diastolic dysfunction. This was a prospective case-control study conducted over a 3-year period involving 29 preterm fetal growth-restricted pregnancies, 25 preeclamptic with fetal growth restriction pregnancies, and 58 matched control pregnancies. Women were assessed by conventional echocardiography and tissue Doppler imaging at diagnosis of the complication and followed-up at 12 weeks postpartum. Fetal growth-restricted pregnancies are characterized by a lower cardiac index and higher total vascular resistance index than expected for gestation. Compared with controls, fetal growth-restricted pregnancy was associated with significantly increased prevalence (PϽ0.001) of asymptomatic left ventricular diastolic dysfunction (28% versus 4%) and widespread impaired myocardial relaxation (59% versus 21%). Unlike preeclampsia, cardiac geometry and intrinsic myocardial contractility were preserved in fetal growth-restricted pregnancy. Fetal growth-restricted pregnancies are characterized by a low output, high resistance circulatory state, as well as a higher prevalence of asymptomatic global diastolic dysfunction and poor cardiac reserve. These findings may explain the increased long-term cardiovascular risk in these women who have had fetal growth-restricted pregnancies. Further studies are needed to clarify the postnatal natural history of cardiac dysfunction in these women. 1,2 FGR and PE are both also associated with increased risk for the long-term development of metabolic syndrome and cardiovascular disease in the mother.3-9 Acute PE is associated with cardiac remodeling, impaired myocardial relaxation and global left ventricular (LV) diastolic chamber dysfunction.10,11 Furthermore, it is evident that the cardiovascular implications of PE do not cease with the birth of the infant, with a significant proportion of women demonstrating asymptomatic LV diastolic chamber dysfunction and essential hypertension for within 2 years of delivery.11,12 Despite these cardiovascular findings in PE, previous studies of maternal cardiac function in FGR pregnancy failed to identify a clear pattern of myocardial impairment or chamber dysfunction. [13][14][15][16] This is possibly due to the inadequacy of the load-dependent indices used and the interpretation of diastolic measures in isolation, disregarding the interdependency of cardiac events. The aim of this study was to test the hypothesis that women with normotensive FGR pregnancies also exhibit cardiac remodeling and myocardial and ventricular dysfunction, as seen in PE pregnanci...

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Section: Melchiorre Et Al Maternal Cardiac Function In Fgr Pregnanciesmentioning

confidence: 81%

Maternal Cardiovascular Impairment in Pregnancies Complicated by Severe Fetal Growth Restriction

et al. 2012

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“…In the present study we focused on the effects of leptin on endothelial dysfunction, a major precursor and contributor of cardiovascular disease and a key feature of obesity, 1,40,49 and on cardiac fibrosis, another characteristic of the obese phenotype and major precursor to heart failure, atrial arrhythmias, and sudden cardiac death. 50,51 We reported for the first time that both leptin-mediated endothelial dysfunction 49 and leptin-associated increases in cardiac fibrotic markers 50 involve mineralocorticoid receptors activation. Indeed, mineralocorticoid receptors antagonism with spironolactone prevented the reduction in endothelium-dependent relaxation induced by chronic leptin treatment.…”

Section: Discussionmentioning

confidence: 98%

“…Similarly, we showed that mineralocorticoid receptors antagonism prevented leptin-induced increases in the expression of collagen 1α1, collagen 3α1, and periostin, three profibrotic markers. This suggests that leptin-induced cardiac fibrosis 50,51 involves mineralocorticoid receptor-dependent mechanisms. Together these data present leptin-mediated increases in aldosterone as a detrimental mechanism for the cardiovascular system and as a major risk factor for cardiovascular disease in the obese population.…”

Section: Discussionmentioning

confidence: 99%

Adipocyte-Derived Hormone Leptin Is a Direct Regulator of Aldosterone Secretion, Which Promotes Endothelial Dysfunction and Cardiac Fibrosis

et al. 2015

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Background-In obesity, the excessive synthesis of aldosterone contributes to the development and progression of metabolic and cardiovascular dysfunctions. Obesity-induced hyperaldosteronism is independent of the known regulators of aldosterone secretion, but reliant on unidentified adipocyte-derived factors. We hypothesized that the adipokine leptin is a direct regulator of aldosterone synthase (CYP11B2) expression and aldosterone release and promotes cardiovascular dysfunction via aldosterone-dependent mechanisms. Methods and Results-Immunostaining of human adrenal cross-sections and adrenocortical cells revealed that adrenocortical cells coexpress CYP11B2 and leptin receptors. Measurements of adrenal CYP11B2 expression and plasma aldosterone levels showed that increases in endogenous (obesity) or exogenous (infusion) leptin dose-dependently raised CYP11B2 expression and aldosterone without elevating plasma angiotensin II, potassium or corticosterone. Neither angiotensin II receptors blockade nor α and β adrenergic receptors inhibition blunted leptin-induced aldosterone secretion. Identical results were obtained in cultured adrenocortical cells. Enhanced leptin signaling elevated CYP11B2 expression and plasma aldosterone, whereas deficiency in leptin or leptin receptors blunted obesity-induced increases in CYP11B2 and aldosterone, ruling out a role for obesity per se. Leptin increased intracellular calcium, elevated calmodulin and calmodulinkinase II expression, whereas calcium chelation blunted leptin-mediated increases in CYP11B2, in adrenocortical cells. Mineralocorticoid receptor blockade blunted leptin-induced endothelial dysfunction and increases in cardiac fibrotic markers. Conclusions-Leptin is a newly described regulator of aldosterone synthesis that acts directly on adrenal glomerulosa cells to increase CYP11B2 expression and enhance aldosterone production via calcium-dependent mechanisms. Furthermore, leptin-mediated aldosterone secretion contributes to cardiovascular disease by promoting endothelial dysfunction and the expression of profibrotic markers in the heart.

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“…Whether fibroblast-specific effects of leptin mediate myocardial fibrosis in obesity has not been rigorously tested. However, exogenous leptin administration in ob/ob mice significantly increased myocardial collagen content promoting matrix-preserving actions (110). …”

Section: The Molecular Signals Regulating Obesity-associated Fibrosismentioning

confidence: 99%

Obesity, metabolic dysfunction, and cardiac fibrosis: pathophysiological pathways, molecular mechanisms, and therapeutic opportunities

Cavalera

Wang

Frangogiannis

2014

Translational Research

209

155

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Cardiac fibrosis is strongly associated with obesity and metabolic dysfunction and may contribute to the increased incidence of heart failure, atrial arrhythmias and sudden cardiac death in obese subjects. Our review discusses the evidence linking obesity and myocardial fibrosis in animal models and human patients, focusing on the fundamental pathophysiologic alterations that may trigger fibrogenic signaling, the cellular effectors of fibrosis and the molecular signals that may regulate the fibrotic response. Obesity is associated with a wide range of pathophysiologic alterations (such as pressure and volume overload, metabolic dysregulation, neurohumoral activation and systemic inflammation); their relative role in mediating cardiac fibrosis is poorly defined. Activation of fibroblasts likely plays a major role in obesity-associated fibrosis; however, inflammatory cells, cardiomyocytes and vascular cells may also contribute to fibrogenic signaling. Several molecular processes have been implicated in regulation of the fibrotic response in obesity. Activation of the Renin-Angiotensin-Aldosterone System, induction of Transforming Growth Factor-β, oxidative stress, advanced glycation end-products (AGEs), endothelin-1, Rho-kinase signaling, leptin-mediated actions and upregulation of matricellular proteins (such as thrombospondin-1) may play a role in the development of fibrosis in models of obesity and metabolic dysfunction. Moreover, experimental evidence suggests that obesity and insulin resistance profoundly affect the fibrotic and remodeling response following cardiac injury. Understanding the pathways implicated in obesity-associated fibrosis may lead to development of novel therapies to prevent heart failure and to attenuate post-infarction cardiac remodeling in obese patients.

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Leptin’s regulation of obesity-induced cardiac extracellular matrix remodeling

Cited by 54 publications

References 32 publications

Maternal Cardiovascular Impairment in Pregnancies Complicated by Severe Fetal Growth Restriction

Maternal Cardiovascular Impairment in Pregnancies Complicated by Severe Fetal Growth Restriction

Adipocyte-Derived Hormone Leptin Is a Direct Regulator of Aldosterone Secretion, Which Promotes Endothelial Dysfunction and Cardiac Fibrosis

Obesity, metabolic dysfunction, and cardiac fibrosis: pathophysiological pathways, molecular mechanisms, and therapeutic opportunities

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