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W2997366394 abstract "The renin angiotensin system (RAS) regulates fluid balance, blood pressure and maintains vascular tone. The potent vasoconstrictor angiotensin II (Ang II) produced by angiotensin-converting enzyme (ACE) comprises the classical RAS. The non-classical RAS involves the conversion of Ang II via ACE2 into the vasodilator Ang (1-7) to counterbalance the effects of Ang II. Furthermore, ACE2 converts AngA into another vasodilator named alamandine. The over activation of the classical RAS (increased vasoconstriction) and depletion of the non-classical RAS (decreased vasodilation) results in vascular dysfunction. Vascular dysfunction is the leading cause of atherosclerosis and cardiovascular disease (CVD). Additionally, local RAS is expressed in various tissues and regulates cellular functions. RAS dysregulation is involved in other several diseases such as inflammation, renal dysfunction and even cancer growth. An approach in restoring vascular dysfunction and other pathological diseases is to either increase the activity of ACE2 or reduce the effect of the classical RAS by counterbalancing Ang II effects. The antitrypanosomal agent, diminazene aceturate (DIZE), is one approach in activating ACE2. DIZE has been shown to exert beneficial effects in CVD experimental models of hypertension, myocardial infarction, type 1 diabetes and atherosclerosis. Thus, this review focuses on DIZE and its effect in several tissues such as blood vessels, cardiac, renal, immune and cancer cells." @default.
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W2997366394 date "2020-01-28" @default.
W2997366394 modified "2023-10-10" @default.
W2997366394 title "The potential actions of angiotensin‐converting enzyme II (ACE2) activator diminazene aceturate (DIZE) in various diseases" @default.
W2997366394 cites W1592232168 @default.
W2997366394 cites W166189507 @default.
W2997366394 cites W1805625916 @default.
W2997366394 cites W1808270696 @default.
W2997366394 cites W1856639763 @default.
W2997366394 cites W1914682693 @default.
W2997366394 cites W1976666772 @default.
W2997366394 cites W1985181577 @default.
W2997366394 cites W1987046124 @default.
W2997366394 cites W1990635146 @default.
W2997366394 cites W1991995202 @default.
W2997366394 cites W2000040025 @default.
W2997366394 cites W2008054951 @default.
W2997366394 cites W2015319932 @default.
W2997366394 cites W2022279911 @default.
W2997366394 cites W2022509884 @default.
W2997366394 cites W2024263079 @default.
W2997366394 cites W2036194057 @default.
W2997366394 cites W2042289853 @default.
W2997366394 cites W2043777410 @default.
W2997366394 cites W2045694929 @default.
W2997366394 cites W2047796919 @default.
W2997366394 cites W2060898700 @default.
W2997366394 cites W2067946831 @default.
W2997366394 cites W2079729786 @default.
W2997366394 cites W2080666283 @default.
W2997366394 cites W2082943727 @default.
W2997366394 cites W2085855084 @default.
W2997366394 cites W2091934488 @default.
W2997366394 cites W2113801726 @default.
W2997366394 cites W2119768071 @default.
W2997366394 cites W2124460853 @default.
W2997366394 cites W2124860950 @default.
W2997366394 cites W2127877077 @default.
W2997366394 cites W2145221672 @default.
W2997366394 cites W2161399617 @default.
W2997366394 cites W2165753570 @default.
W2997366394 cites W2166343963 @default.
W2997366394 cites W2248269212 @default.
W2997366394 cites W2253167126 @default.
W2997366394 cites W2325452586 @default.
W2997366394 cites W2337247222 @default.
W2997366394 cites W2467869866 @default.
W2997366394 cites W2497451167 @default.
W2997366394 cites W2589308094 @default.
W2997366394 cites W2614020568 @default.
W2997366394 cites W2740033396 @default.
W2997366394 cites W2744925671 @default.
W2997366394 cites W2755043911 @default.
W2997366394 cites W2774046602 @default.
W2997366394 cites W2784925193 @default.
W2997366394 cites W2797452440 @default.
W2997366394 cites W2802009617 @default.
W2997366394 cites W2883052031 @default.
W2997366394 cites W2886434849 @default.
W2997366394 cites W2890659492 @default.
W2997366394 cites W2893187431 @default.
W2997366394 cites W2946455326 @default.
W2997366394 cites W4246390714 @default.
W2997366394 doi "https://doi.org/10.1111/1440-1681.13251" @default.
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