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Reproducibility and observer variability of tissue phase mapping for the quantification of regional myocardial velocities
Authors:Kai Lin  Varun Chowdhary  Keith H. Benzuly  Clyde W. Yancy  Jon W. Lomasney  Vera H. Rigolin  Allen S. Anderson  Jane Wilcox  James Carr  Michael Markl
Affiliation:1.Department of Radiology, Feinberg School of Medicine,Northwestern University,Chicago,USA;2.Division of Cardiology, Department of Medicine, Feinberg School of Medicine,Northwestern University,Chicago,USA;3.Department of Pathology and Pharmacology, Feinberg School of Medicine,Northwestern University,Chicago,USA;4.Department of Biomedical Engineering, McCormick School of Engineering,Northwestern University,Evanston,USA
Abstract:To systematically investigate the reproducibility of global and segmental left ventricular (LV) velocities derived from tissue phase mapping (TPM). Breath held and ECG synchronized TPM data (spatial/temporal resolution?=?2?×?2 mm2/20.8 ms) were acquired in 18 healthy volunteers. To analyze scan–rescan variability, TPM was repeated in all subjects during a second visit separated by 16?±?5 days. Data analysis included LV segmentation, and quantification of global and regional (AHA 16-segment modal) metrics of LV function [velocity–time curves, systolic and diastolic peak and time-to-peak (TTP) velocities] for radial (Vr), long-axis (Vz) and circumferential (VΦ) LV velocities. Mean velocity time curves in basal, mid-ventricular, and apical locations showed highly similar LV motion patterns for all three velocity components (Vr, VΦ, Vz) for scan and rescan. No significant differences for both systolic and diastolic peak and TTP myocardial velocities were observed. Segmental analysis revealed similar regional peak Vr and Vz during both systole and diastole except for three LV segments (p?=?0.045, p?=?0.033, and p?=?0.009). Excellent (p?2?=?0.92), peak Vz (R2?=?0.90), radial TTP (R2?=?0.91) and long-axis TTP (R2?=?0.88) confirmed good agreement. Bland–Altman analysis demonstrated excellent intra-observer and good inter-observer analysis agreement but increased variability for long axis peak velocities. TPM based analysis of global and regional myocardial velocities can be performed with good reproducibility. Robustness of regional quantification of long-axis velocities was limited but spatial velocity distributions across the LV could reliably be replicated.
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