Cardiac kallikrein-kinin system is upregulated in chronic volume overload and mediates an inflammatory induced collagen loss

Cardiac kallikrein-kinin system is upregulated in chronic volume overload and mediates an inflammatory induced collagen loss

The clinical problem of a "pure volume overload" as in isolated mitral or aortic regurgitation currently has no documented medical therapy that attenuates collagen loss and the resultant left ventricular (LV) dilatation and failure. Here, we identify a potential mechanism related to upregu...

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Bibliographic Details
Published in:PloS one Vol. 7; no. 6; p. e40110
Main Authors: Wei, Chih-Chang, Chen, Yuanwen, Powell, Lindsay C, Zheng, Junying, Shi, Ke, Bradley, Wayne E, Powell, Pamela C, Ahmad, Sarfaraz, Ferrario, Carlos M, Dell'Italia, Louis J
Format: Journal Article
Language:English
Published: United States Public Library of Science 29-06-2012
Public Library of Science (PLoS)
Subjects:
Age
Angiotensin II - blood
Animals
Aorta
Aprotinin - pharmacology
Biology
Blood pressure
Bradykinin
Bradykinin - blood
Cardiomyocytes
Cardiovascular disease
Catecholamines - blood
Cell Count
Cell Degranulation - drug effects
Chymase
Chymases - metabolism
Collagen
Collagen - metabolism
Diastolic pressure
Echocardiography
Enzymes
Extracellular Fluid
Extracellular matrix
Fibroblasts
Fistulae
Gelatinase
Gelatinases - metabolism
Gene expression
Heart
Heart diseases
Heart failure
Heart Ventricles - diagnostic imaging
Heart Ventricles - enzymology
Heart Ventricles - pathology
Heart Ventricles - physiopathology
Hemodynamics
Hemodynamics - drug effects
Hypertension
Immunohistochemistry
Infiltration
Inflammation
Inflammation - complications
Inflammation - genetics
Inflammation - pathology
Inhibitors
Kallikrein
Kallikrein-Kinin System - drug effects
Mast cells
Mast Cells - drug effects
Mast Cells - enzymology
Mast Cells - physiology
Medicine
Models, Cardiovascular
Myocardium - metabolism
Myocardium - pathology
Peptidyl-Dipeptidase A - genetics
Peptidyl-Dipeptidase A - metabolism
Rats
Receptors, Bradykinin - metabolism
Regurgitation
RNA
RNA, Messenger - genetics
RNA, Messenger - metabolism
Rodents
Ultrasonography
Up-Regulation - drug effects
Vascular Fistula - diagnostic imaging
Vascular Fistula - genetics
Vascular Fistula - pathology
Vascular Fistula - physiopathology
Ventricle
Ventricular Remodeling - drug effects
North Carolina
Alabama
United States > US
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Summary:The clinical problem of a "pure volume overload" as in isolated mitral or aortic regurgitation currently has no documented medical therapy that attenuates collagen loss and the resultant left ventricular (LV) dilatation and failure. Here, we identify a potential mechanism related to upregulation of the kallikrein-kinin system in the volume overload of aortocaval fistula (ACF) in the rat. LV interstitial fluid (ISF) collection, hemodynamics, and echocardiography were performed in age-matched shams and 4 and 15 wk ACF rats. ACF rats had LV dilatation and a 2-fold increase in LV end-diastolic pressure, along with increases in LV ISF bradykinin, myocardial kallikrein and bradykinin type-2 receptor (BK(2)R) mRNA expression. Mast cell numbers were increased and interstitial collagen was decreased at 4 and 15 wk ACF, despite increases in LV ACE and chymase activities. Treatment with the kallikrein inhibitor aprotinin preserved interstitial collagen, prevented the increase in mast cells, and improved LV systolic function at 4 wk ACF. To establish a cause and effect between ISF bradykinin and mast cell-mediated collagen loss, direct LV interstitial bradykinin infusion in vivo for 24 hrs produced a 2-fold increase in mast cell numbers and a 30% decrease in interstitial collagen, which were prevented by BK(2)R antagonist. To further connect myocardial stretch with cellular kallikrein-kinin system upregulation, 24 hrs cyclic stretch of adult cardiomyocytes and fibroblasts produced increased kallikrein, BK(2)R mRNA expressions, bradykinin protein and gelatinase activity, which were all decreased by the kallikrein inhibitor-aprotinin. A pure volume overload is associated with upregulation of the kallikrein-kinin system and ISF bradykinin, which mediates mast cell infiltration, extracellular matrix loss, and LV dysfunction-all of which are improved by kallikrein inhibition. The current investigation provides important new insights into future potential medical therapies for the volume overload of aortic and mitral regurgitation.
Bibliography:Conceived and designed the experiments: CCW LJD. Performed the experiments: CCW YC LCP JZ KS WEB PCP SA. Analyzed the data: CCW CMF LJD. Contributed reagents/materials/analysis tools: CCW SA CMF LJD. Wrote the paper: CCW LJD.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0040110