Published online before print August 20, 2007, doi: 10.1161/CIRCULATIONAHA.107.707737
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(Circulation. 2007;116:1250-1257.)
© 2007 American Heart Association, Inc.
Imaging |
In Vivo Characterization of Murine Myocardial Perfusion With Myocardial Contrast Echocardiography
Validation and Application in Nitric Oxide Synthase 3–Deficient Mice
From the Cardiac Ultrasound Laboratory in the Cardiology Division of the Department of Medicine (M.J.R., H.T., K.K.P., M.H.P., M.S.-C.), the Cardiovascular Research Center (M.J.R., H.T., K.D.B., M.S.-C.), the Department of Anesthesia and Critical Care (M.J.R., R.L., F.I., W.M.Z., K.D.B.), and the Institute for Technology Assessment (E.F.H.), Massachusetts General Hospital and Harvard Medical School, Boston, Mass; and INSERM E 0226 (H.T., G.D.), Université Claude Bernard Lyon I, Lyon, France.
Correspondence to Marielle Scherrer-Crosbie, MD, PhD, Cardiac Ultrasound Laboratory, Massachusetts General Hospital, 55 Fruit St, Boston, MA 02114. E-mail marielle{at}crosbie.com
Received November 4, 2006; accepted June 29, 2007.
Background— The ability to noninvasively evaluate murine myocardial blood flow (MBF) in vivo would provide an important tool for cardiovascular research. Myocardial contrast echocardiography (MCE) has been used to measure MBF; however, it has not been validated in mice. This study assesses whether MCE can evaluate MBF at rest and after vasodilation and measure the maximal augmentation (coronary reserve) of MBF in mice. Wild-type (WT) and nitric oxide synthase 3 (NOS3)–deficient (NOS3–/–) mice were studied.
Methods and Results— MCE was performed at baseline and after intravenous infusion of acetylcholine or adenosine. Definity contrast agent was infused, and parasternal views were acquired in real-time mode. Replenishment curves of myocardial contrast were obtained, and rates of signal rise (ß) and plateau intensity (A) were calculated. MBF estimated by the product of A and ß (Aß) was compared with that measured with fluorescent microspheres. MCE analysis was feasible in 98% (52/53) of mice. MBF measured by microspheres increased with adenosine and correlated closely with Aß. There was no difference in MCE-derived MBF between WT and NOS3–/– mice at rest. Adenosine infusion increased MBF by 3.0±0.6-fold in NOS3–/– mice and 2.5±0.3-fold in WT (P=0.58 between genotypes). Acetylcholine induced an increase of 2.4±0.2-fold in MBF in WT mice but did not increase MBF in NOS3–/– mice (P<0.0005 versus WT).
Conclusions— MBF, coronary reserve, and vasodilator responses can be evaluated accurately in the intact mouse by MCE. This method demonstrated a preserved coronary response to adenosine but an impaired acetylcholine-induced vasodilation in NOS3–/– mice compared with WT mice.
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