Should increasing the dose or adding an AT1 receptor blocker follow a relatively low dose of ACE inhibitor initiated in acute myocardial infarction?

doi:10.1016/S0008-6363(03)00318-3

Cardiovascular Research 2003 58(3):611-620; doi:10.1016/S0008-6363(03)00318-3
© 2003 by European Society of Cardiology

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Should increasing the dose or adding an AT₁ receptor blocker follow a relatively low dose of ACE inhibitor initiated in acute myocardial infarction?

Tadashi Sugie^a, Yutaka Kagaya^a, Morihiko Takeda^a, Hirokazu Yahagi^a, Chikako Takahashi^a, Jun Takahashi^a, Mototsugu Ninomiya^a, Jun Watanabe^a, Ryo Ichinohasama^b, Fumiaki Tezuka^c and Kunio Shirato^a^,*

^aDepartment of Cardiovascular Medicine, Tohoku University Graduate School of Medicine, 1-1 Seiryo-machi, Aoba-ku, Sendai 980-8574, Japan
^bDepartment of Oral Pathology, Tohoku University Graduate School of Dentistry, Sendai, Japan
^cNational Sendai Hospital, Sendai, Japan

shirato{at}int1.med.tohoku.ac.jp

^* Corresponding author. Tel.: +81-22-717-7153; fax: +81-22-717-7156.

Objective: Based on currently available clinical evidence, weshould use high-dose angiotensin converting enzyme inhibitor(ACE-I) for patients with acute myocardial infarction (MI),initiating it at incremental doses to avoid excessive hypotension.Recent animal studies with acute MI models failed to demonstratethe superiority of the combination therapy of ACE-I and angiotensinreceptor blocker (ARB) to high-dose ACE-I treatment with comparableblood pressure reductions, which however might be attributedto the initiation of the targeted doses from the beginning.The aim of this study was to compare the effect of increasingthe dose of ACE-I with that of adding ARB following a relativelylow dose of ACE-I on the survival and left ventricular (LV)remodeling after MI. Methods: Rats underwent left coronary arteryligation and were treated with either ACE-I temocapril (5 mg/kg/day)or vehicle for 2 weeks, which was initiated 3 days after thesurgery. The rats treated with temocapril were further randomlyassigned to receive either high-dose temocapril (10 mg/kg/day)or combination therapy (temocapril 5 mg/kg/day+olmesartan 2.5mg/kg/day), which was continued for another 6 weeks. Results:Both treatments similarly reduced the blood pressure, improvedsurvival and ameliorated LV enlargement. In contrast, severalparameters of LV function were significantly ameliorated onlyby the high-dose ACE-I but not by the combination therapy. Conclusions:After the initiation of a relatively low dose of ACE-I in acuteMI, increasing the dose of ACE-I or adding ARB may equally improvesurvival and LV remodeling in the setting of an equal hypotensiveeffect. Further study with a longer treatment protocol is requiredto determine whether the several favorable effects on LV functionelicited only by the high-dose ACE-I treatment provide furtherbeneficial effects on survival and LV remodeling compared withthe combination therapy.

KEYWORDS ACE inhibitors; Infarction; Remodeling; Renin angiotensin system; Ventricular function

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