PAI-1 protects mice from hypertension-induced cardiac fibrosis by inhibiting the urokinase-mediated generation of active plasmin.
PAI-1 protects mice from hypertension-induced cardiac fibrosis by inhibiting the generation of active plasmin.
Abstract Plasminogen activator inhibitor-1 (PAI-1) is known to protect mice against cardiac fibrosis. It has been speculated that PAI-1 may regulate cardiac fibrosis by inactivating urokinase-type plasminogen activator (uPA) and ultimately plasmin (Pm) generation. However, the in vivo role of PAI-1 in inactivating uPA and limiting the generation of Pm during cardiac fibrosis remains to be established. The objective of this study was to determine if the cardioprotective effect of PAI-1 is mediated through its ability to directly regulate urokinase -mediated activation of plasminogen (Pg). An Angiotensin II (AngII)-aldosterone (Ald) infusion mouse model of hypertension was utilised in this study. Four weeks after AngII-Ald infusion, PAI-1-deficient (PAI-1 −/− ) mice developed severe cardiac fibrosis. However, a marked reduction in cardiac fibrosis was observed in PAI-1 −/− /uPA −/− double knockout mice that was associated with reduced inflammation, lower expression levels of TGF-β and proteases associated with tissue remodeling, and diminished Smad2 signaling. Moreover, total ablation of cardiac fibrosis was observed in PAI-1 −/− mice that express inactive plasmin (Pm) but normal levels of zymogen Pg (PAI-1 −/− /Pg S743A/S743A ). Our findings indicate that PAI-1 protects mice from hypertension-induced cardiac fibrosis by inhibiting the generation of active Pm.
Gupta et al. (Fri,) conducted a other in Hypertension-induced cardiac fibrosis. PAI-1 deficiency and uPA/plasmin genetic modifications vs. PAI-1 -/- mice vs PAI-1 -/- / uPA -/- double knockout and PAI-1 -/- / Pg S743A/S743A mice was evaluated on Cardiac fibrosis. PAI-1 protects mice from hypertension-induced cardiac fibrosis by inhibiting the urokinase-mediated generation of active plasmin.
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