Elasticity-based determination of isovolumetric phases in the human heart

Background/motivation. to directly determine isovolumetric cardiac time intervals by magnetic resonance elastography (mre) using the magnitude of the complex signal for deducing morphological information combined with the phase of the complex signal for tension-relaxation measurements. methods. thirty-five healthy volunteers and 11 patients with relaxation abnormalities were subjected to transthoracic wave stimulation using vibrations of approximately 25 hz. a k-space-segmented,ecg-gated gradient-recalled echo steady-state sequence with a 500-hz bipolar motion-encoding gradient was used for acquiring a series of 360 complex images of a short-axis view of the heart at a frame rate of less than 5.2 ms. magnitude images were employed for measuring the cross-sectional area of the left ventricle,while phase images were used for analyzing the amplitudes of the externally induced waves. the delay between the decrease in amplitude and onset of ventricular contraction was determined in all subjects and assigned to the time of isovolumetric tension. conversely,the delay between the increase in wave amplitude and ventricular dilatation was used for measuring the time of isovolumetric elasticity relaxation. results: wave amplitudes decreased during systole and increased during diastole. the variation in wave amplitude occurred ahead of morphological changes. in healthy volunteers the time of isovolumetric elasticity relaxation was 75 31 ms,which is significantly shorter than the time of isovolumetric tension of 136 36 ms (p < 0.01). in patients with relaxation abnormalities (mild diastolic dysfunction,n = 11) isovolumetric elasticity relaxation was significantly prolonged,with 133 57 ms (p < 0.01),whereas isovolumetric tension time was in the range of healthy controls (161 45 ms; p = 0.053). conclusion: the complex mre signal conveys complementary information on cardiac morphology and elasticity,which can be combined for directly measuring isovolumetric tension and elasticity relaxation in the human heart. © 2010 elgeti et al; licensee biomed central ltd.