Activation pattern of ACE2/Ang-(1–7) and ACE/Ang II pathway in course of heart failure assessed by multiparametric MRI in vivo in Tgαq*44 mice

Tyrankiewicz, Urszula; Olkowicz, Mariola; Skórka, Tomasz; Jabłońska, Magdalena; Orzyłowska, Anna; Bar, Anna; Gonet, Michał; Berkowicz, Piotr; Jasiński, K; Zoladz, Jerzy A.; Smolenski, Ryszard T.; Chłopicki, Stefan

doi:10.1152/japplphysiol.00571.2017

Cited by 18 publications

(45 citation statements)

References 59 publications

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“…As early as the fourth month, mRNA for the β‐myosin heavy chain is expressed in cardiomyocytes, indicating activation of fetal genes; cardiac fibrosis is already 4‐fold higher compared to control mice—indicating pathological tissue reorganization and increased compensatory expression of cardiomyocyte desmin, subsequently resulting in extracellular matrix remodeling and sarcomere pathological reorganization as in mechanical stress . Altogether, cardiomyocyte pathology in Tgαq*44 mice, while maintaining normotension, leads to slowly progressing heart deterioration and HF that was previously characterized, but it was not known whether HF in this model results in VCI.…”

Section: Discussionmentioning

confidence: 83%

“…At the age of 6 months, Tgαq*44 mouse heart function parameters are lower (EF=59%, CO=14.4 mL/min, preserved high‐dose dobutamine response), but global cardiac function is still fully maintained. Yet, at this stage we detect changes characteristic for atrial pathology—lower atrial late flow velocity and subtle diastolic dysfunction of LV—detectable only as decreased myocardial radial strain but not as hemodynamic parameter changes (EF/CO) . At 10 months, global cardiac performance is decreased (ejection rate, fraction area change) .…”

Section: Methodsmentioning

confidence: 80%

“…Yet, at this stage we detect changes characteristic for atrial pathology—lower atrial late flow velocity and subtle diastolic dysfunction of LV—detectable only as decreased myocardial radial strain but not as hemodynamic parameter changes (EF/CO) . At 10 months, global cardiac performance is decreased (ejection rate, fraction area change) . Therefore, Tgαq*44 mice at the ages of 3, 6, and 10 months represent sequential stages of heart failure development: normal heart, early diastolic, and systolic/diastolic cardiac dysfunction, respectively.…”

Section: Methodsmentioning

confidence: 84%

“…Therefore, Tgαq*44 mice at the ages of 3, 6, and 10 months represent relatively early stages of HF development. At the age of 4 months, Tgαq*44 mice have preserved global cardiac function (EF=63%, cardiac output [CO]=15 mL/min, preserved high‐dose dobutamine response) and show no functional difference from age‐matched control FVB mice; hence, younger‐than‐3‐month Tgαq*44 mice represent a functionally normal heart . At the age of 6 months, Tgαq*44 mouse heart function parameters are lower (EF=59%, CO=14.4 mL/min, preserved high‐dose dobutamine response), but global cardiac function is still fully maintained.…”

Section: Methodsmentioning

confidence: 99%

“…In this study we assessed (1) whether slowly progressing heart pathology—before the development of LV systolic dysfunction and end‐stage HF—leads to VCI, and (2) what roles the 2 previously proposed major cardiac pathomechanisms—global cerebral hypoperfusion and prothrombotic condition—play in VCI development. We employed Tgαq*44 mice in which HF develops due to slowly progressing cardiomyopathy, which mimics human HF on a molecular, morphological, phenotypic, and functional level . Their pathology is triggered by postnatal activation of a cardiomyocyte‐specific transgene, causing agonist‐independent, constitutive activation of the Gαq pathway, present only in cardiomyocytes .…”

mentioning

confidence: 99%

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Vascular Cognitive Impairment Linked to Brain Endothelium Inflammation in Early Stages of Heart Failure in Mice

Adamski

Sternak

Mohaissen

et al. 2018

JAHA

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BackgroundAlthough advanced heart failure (HF) is a clinically documented risk factor for vascular cognitive impairment, the occurrence and pathomechanisms of vascular cognitive impairment in early stages of HF are equivocal. Here, we characterize vascular cognitive impairment in the early stages of HF development and assess whether cerebral hypoperfusion or prothrombotic conditions are involved.Methods and ResultsTgαq*44 mice with slowly developing isolated HF triggered by cardiomyocyte‐specific overexpression of G‐αq*44 protein were studied before the end‐stage HF, at the ages of 3, 6, and 10 months: before left ventricle dysfunction; at the stage of early left ventricle diastolic dysfunction (with preserved ejection fraction); and left ventricle diastolic/systolic dysfunction, respectively. In 6‐ to 10‐month‐old but not in 3‐month‐old Tgαq*44 mice, behavioral and cognitive impairment was identified with compromised blood‐brain barrier permeability, most significantly in brain cortex, that was associated with myelin sheet loss and changes in astrocytes and microglia. Brain endothelial cells displayed increased E‐selectin immunoreactivity, which was accompanied by increased amyloid‐β1‐42 accumulation in piriform cortex and increased cortical oxidative stress (8‐OHdG immunoreactivity). Resting cerebral blood flow measured by magnetic resonance imaging in vivo was preserved, but ex vivo NO‐dependent cortical arteriole flow regulation was impaired. Platelet hyperreactivity was present in 3‐ to 10‐month‐old Tgαq*44 mice, but it was not associated with increased platelet‐dependent thrombogenicity.ConclusionsWe report for the first time that vascular cognitive impairment is already present in the early stage of HF development, even before left ventricle systolic dysfunction. The underlying pathomechanism, independent of brain hypoperfusion, involves preceding platelet hyperreactivity and brain endothelium inflammatory activation.

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