Maggie Fung
GE Healthcare
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Publication
Featured researches published by Maggie Fung.
Circulation | 2008
Srinivas R. Dukkipati; Richard Philip Mallozzi; Ehud J Schmidt; Godtfred Holmvang; Andre d'Avila; Renee Guhde; Robert David Darrow; Glenn S. Slavin; Maggie Fung; Zachary J. Malchano; Greg Kampa; Jeremy D. Dando; Christina D. McPherson; Thomas Kwok-Fah Foo; Jeremy N. Ruskin; Charles Lucian Dumoulin; Vivek Y. Reddy
Background— X-ray fluoroscopy constitutes the fundamental imaging modality for catheter visualization during interventional electrophysiology procedures. The minimal tissue discriminative capability of fluoroscopy is mitigated in part by the use of electroanatomic mapping systems and enhanced by the integration of preacquired 3-dimensional imaging of the heart with computed tomographic or magnetic resonance (MR) imaging. A more ideal paradigm might be to use intraprocedural MR imaging to directly image and guide catheter mapping procedures. Methods and Results— An MR imaging–based electroanatomic mapping system was designed to assess the feasibility of navigating catheters to the left ventricle in vivo using MR tracking of microcoils incorporated into the catheters, measuring intracardiac ventricular electrograms, and integrating this information with 3-dimensional MR angiography and myocardial delayed enhancement images to allow ventricular substrate mapping. In all animals (4 normal, and 10 chronically infarcted swine), after transseptal puncture under fluoroscopic guidance, catheters were successfully navigated to the left ventricle with MR tracking (13 to 15 frames per second) by both transseptal and retrograde aortic approaches. Electrogram artifacts related to the MR imaging gradient pulses were successfully removed with analog and digital signal processing. In all animals, it was possible to map the entire left ventricle and to project electrogram voltage amplitude maps to identify the scarred myocardium. Conclusions— It is possible to use MR tracking to navigate catheters to the left ventricle, to measure electrogram activity, and to render accurate 3-dimensional voltage maps in a porcine model of chronic myocardial infarction, completely in the MR imaging environment. Myocardial delayed enhancement guidance provided dense sampling of the proximity of the infarct and accurate localization of complex infarcts.
Circulation-arrhythmia and Electrophysiology | 2009
Ehud J. Schmidt; Richard Philip Mallozzi; Aravinda Thiagalingam; Godtfred Holmvang; Andre d'Avila; Renee Guhde; Robert David Darrow; Glenn S. Slavin; Maggie Fung; Jeremy D. Dando; Lori Foley; Charles Lucian Dumoulin; Vivek Y. Reddy
Background—The MRI-compatible electrophysiology system previously used for MR-guided left ventricular electroanatomic mapping was enhanced with improved MR tracking, an MR-compatible radiofrequency ablation system and higher-resolution imaging sequences to enable mapping, ablation, and ablation monitoring in smaller cardiac structures. MR-tracked navigation was performed to the left atrium (LA) and atrioventricular (AV) node, followed by LA electroanatomic mapping and radiofrequency ablation of the pulmonary veins (PVs) and AV node. Methods and Results—One ventricular ablation, 7 PV ablations, 3 LA mappings, and 3 AV node ablations were conducted. Three MRI-compatible devices (ablation/mapping catheter, torqueable sheath, stimulation/pacing catheter) were used, each with 4 to 5 tracking microcoils. Transseptal puncture was performed under x-ray, with all other procedural steps performed in the MRI. Preacquired MRI roadmaps served for real-time catheter navigation. Simultaneous tracking of 3 devices was performed at 13 frames per second. LA mapping and PV radiofrequency ablation were performed using tracked ablation catheters and sheaths. Ablation points were registered and verified after ablation using 3D myocardial delayed enhancement and postmortem gross tissue examination. Complete LA electroanatomic mapping was achieved in 3 of 3 pigs, Right inferior PV circumferential ablation was achieved in 3 of 7 pigs, with incomplete isolation caused by limited catheter deflection. During AV node ablation, ventricular pacing was performed, 3 devices were simultaneously tracked, and intracardiac ECGs were displayed. 3D myocardial delayed enhancement visualized node injury 2 minutes after ablation. AV node block succeeded in 2 of 3 pigs, with 1 temporary block. Conclusions—LA mapping, PV radiofrequency ablation, and AV node ablation were demonstrated under MRI guidance. Intraprocedural 3D myocardial delayed enhancement assessed lesion positional accuracy and dimensions.
Journal of Magnetic Resonance Imaging | 2016
Temel Kaya Yasar; Mathilde Wagner; Octavia Bane; Cecilia Besa; James S. Babb; Stephan Kannengiesser; Maggie Fung; Richard L. Ehman
To assess interplatform reproducibility of liver stiffness (LS) and spleen stiffness (SS) measured with magnetic resonance elastography (MRE) based on a 2D gradient echo (GRE) sequence.
Radiology | 2017
Mathilde Wagner; Idoia Corcuera-Solano; G.H. Lo; Steven J. Esses; Joseph Liao; Cecilia Besa; Nelson Chen; Ginu Abraham; Maggie Fung; James S. Babb; Richard L. Ehman
Purpose To assess the determinants of technical failure of magnetic resonance (MR) elastography of the liver in a large single-center study. Materials and Methods This retrospective study was approved by the institutional review board. Seven hundred eighty-one MR elastography examinations performed in 691 consecutive patients (mean age, 58 years; male patients, 434 [62.8%]) in a single center between June 2013 and August 2014 were retrospectively evaluated. MR elastography was performed at 3.0 T (n = 443) or 1.5 T (n = 338) by using a gradient-recalled-echo pulse sequence. MR elastography and anatomic image analysis were performed by two observers. Additional observers measured liver T2* and fat fraction. Technical failure was defined as no pixel value with a confidence index higher than 95% and/or no apparent shear waves imaged. Logistic regression analysis was performed to assess potential predictive factors of technical failure of MR elastography. Results The technical failure rate of MR elastography at 1.5 T was 3.5% (12 of 338), while it was higher, 15.3% (68 of 443), at 3.0 T. On the basis of univariate analysis, body mass index, liver iron deposition, massive ascites, use of 3.0 T, presence of cirrhosis, and alcoholic liver disease were all significantly associated with failure of MR elastography (P < .004); but on the basis of multivariable analysis, only body mass index, liver iron deposition, massive ascites, and use of 3.0 T were significantly associated with failure of MR elastography (P < .004). Conclusion The technical failure rate of MR elastography with a gradient-recalled-echo pulse sequence was low at 1.5 T but substantially higher at 3.0 T. Massive ascites, iron deposition, and high body mass index were additional independent factors associated with failure of MR elastography of the liver with a two-dimensional gradient-recalled-echo pulse sequence.
Investigative Radiology | 2016
Wagner M; Cecilia Besa; Bou Ayache J; Yasar Tk; Octavia Bane; Maggie Fung; Richard L. Ehman
ObjectiveThe aim of this study was to compare 2-dimensional (2D) gradient recalled echo (GRE) and 2D spin echo echoplanar imaging (SE-EPI) magnetic resonance elastography (MRE) sequences of the liver in terms of image quality and quantitative liver stiffness (LS) measurement. Materials and MethodsThis prospective study involved 50 consecutive subjects (male/female, 33/17; mean age, 58 years) who underwent liver magnetic resonance imaging at 3.0 T including 2 MRE sequences, 2D GRE, and 2D SE-EPI (acquisition time 56 vs 16 seconds, respectively). Image quality scores were assessed by 2 independent observers based on wave propagation and organ coverage on the confidence map (range, 0–15). A third observer measured LS on stiffness maps (in kilopascal). Mean LS values, regions of interest size (based on confidence map), and image quality scores between SE-EPI and GRE-MRE were compared using paired nonparametric Wilcoxon test. Reproducibility of LS values between the 2 sequences was assessed using intraclass coefficient correlation, coefficient of variation, and Bland-Altman limits of agreement. T2* effect on image quality was assessed using partial Spearman correlation. ResultsThere were 4 cases of failure with GRE-MRE and none with SE-EPI-MRE. Image quality scores and region of interest size were significantly higher using SE-EPI-MRE versus GRE-MRE (P < 0.0001 for both measurements and observers). Liver stiffness measurements were not significantly different between the 2 sequences (3.75 ± 1.87 kPa vs 3.55 ± 1.51 kPa, P = 0.062), were significantly correlated (intraclass coefficient correlation, 0.909), and had excellent reproducibility (coefficient of variation, 10.2%; bias, 0.023; Bland-Altman limits of agreement, −1.19; 1.66 kPa). Image quality scores using GRE-MRE were significantly correlated with T2* while there was no correlation for SE-EPI-MRE. ConclusionsOur data suggest that SE-EPI-MRE may be a better alternative to GRE-MRE. The diagnostic performance of SE-EPI-MRE for detection of liver fibrosis needs to be assessed in a future study.
Journal of Magnetic Resonance Imaging | 2018
Tina Jeon; Maggie Fung; Kevin M. Koch; Ek Tsoon Tan; Darryl B. Sneag
Diffusion tensor imaging (DTI) is a noninvasive magnetic resonance imaging (MRI) technique that measures the extent of restricted water diffusion and anisotropy in biological tissue. Although DTI has been widely applied in the brain, more recently researchers have used it to characterize nerve pathology in the setting of entrapment neuropathy, traumatic injury, and tumor. DTI artifacts are exacerbated when imaging off isocenter in the body. Anecdotally, the most significant artifacts in peripheral nerve DTI include magnetic field inhomogeneity, motion, incomplete fat suppression, aliasing, and distortion. High spatial resolution is also required to reliably evaluate smaller peripheral nerves. This article provides an overview of such technical issues, particularly when trying to apply DTI in the clinical setting, and offers potential solutions.
Europace | 2014
Ehud J. Schmidt; Maggie Fung; Pelin Aksit Ciris; Ting Song; Ajit Shankaranarayanan; Godtfred Holmvang; Sandeep N. Gupta; Miguel Chaput; Robert A. Levine; Jeremy N. Ruskin; Vivek Y. Reddy; Andre d'Avila; Anthony H. Aletras; Stephan B. Danik
AIMS Prior work has demonstrated that magnetic resonance imaging (MRI) strain can separate necrotic/stunned myocardium from healthy myocardium in the left ventricle (LV). We surmised that high-resolution MRI strain, using navigator-echo-triggered DENSE, could differentiate radiofrequency ablated tissue around the pulmonary vein (PV) from tissue that had not been damaged by radiofrequency energy, similarly to navigated 3D myocardial delayed enhancement (3D-MDE). METHODS AND RESULTS A respiratory-navigated 2D-DENSE sequence was developed, providing strain encoding in two spatial directions with 1.2 × 1.0 × 4 mm(3) resolution. It was tested in the LV of infarcted sheep. In four swine, incomplete circumferential lesions were created around the right superior pulmonary vein (RSPV) using ablation catheters, recorded with electro-anatomic mapping, and imaged 1 h later using atrial-diastolic DENSE and 3D-MDE at the left atrium/RSPV junction. DENSE detected ablation gaps (regions with >12% strain) in similar positions to 3D-MDE (2D cross-correlation 0.89 ± 0.05). Low-strain (<8%) areas were, on average, 33% larger than equivalent MDE regions, so they include both injured and necrotic regions. Optimal DENSE orientation was perpendicular to the PV trunk, with high shear strain in adjacent viable tissue appearing as a sensitive marker of ablation lesions. CONCLUSIONS Magnetic resonance imaging strain may be a non-contrast alternative to 3D-MDE in intra-procedural monitoring of atrial ablation lesions.
Journal of Cardiovascular Magnetic Resonance | 2012
Peng Lai; Maggie Fung; Shreyas S. Vasanawala; Anja C. S. Brau
Summary This work presents a kt acceleration method (kat ARC) for retrospective cardiac-gated 3D cardiac cine MRI. Our in-vivo results show that 3D cine images of the entire ventricle are obtainable within a single breathhold using highly accelerated kat ARC. Background For quantitative volumetric assessments of cardiac function, 3D cine images depicting motion of the entire ventricle in a complete cardiac cycle are needed. However, due to limited acceleration capability, breathheld 3D cine MRI is not obtainable using conventional parallel imaging. Several kt-acceleration methods have demonstrated high-acceleration capability for dynamic MRI by exploiting spatiotemporal correlation [Tsao, MRM 2003; Huang, MRM 2005]. This study aims to investigate the feasibility of breathheld retrospective cardiac-gated whole-ventricle 3D cine MRI using kat ARC (k-adaptive-t Autocalibrating Reconstruction for Cartesian sampling [Lai, ISMRM 2009]). Methods
Journal of Cardiovascular Magnetic Resonance | 2014
Glenn S. Slavin; Maggie Fung
Background Single-phase cardiac MRI acquires data only during a brief period of the cardiac cycle. To avoid motion artifacts, the operator must select a trigger delay that corresponds to a period of minimal cardiac motion, typically at end-systole or mid-diastole. This can be done by inspecting a prior cine scan for quiescent periods. However, because these cardiac phases can vary in temporal position and duration as a function of heart rate, another option should be available if the heart rate at the time of the single-phase scan differs from that during the cine scan. The goal of this work was to analytically determine the optimal trigger delays for cardiac MRI. Methods
Journal of medical imaging | 2017
David C. Newitt; Dariya I. Malyarenko; Thomas L. Chenevert; C. Chad Quarles; Laura C. Bell; Andriy Fedorov; Fiona M. Fennessy; Michael A. Jacobs; Meiyappan Solaiyappan; Stefanie J. C. G. Hectors; Mark Muzi; Paul E. Kinahan; Kathleen M. Schmainda; Melissa Prah; Erin N. Taber; Christopher D. Kroenke; Wei Huang; Lori R. Arlinghaus; Thomas E. Yankeelov; Yue Cao; Madhava P. Aryal; Yi-Fen Yen; Jayashree Kalpathy-Cramer; Amita Shukla-Dave; Maggie Fung; Jiachao Liang; Michael A. Boss; Nola M. Hylton
Abstract. Diffusion weighted MRI has become ubiquitous in many areas of medicine, including cancer diagnosis and treatment response monitoring. Reproducibility of diffusion metrics is essential for their acceptance as quantitative biomarkers in these areas. We examined the variability in the apparent diffusion coefficient (ADC) obtained from both postprocessing software implementations utilized by the NCI Quantitative Imaging Network and online scan time-generated ADC maps. Phantom and in vivo breast studies were evaluated for two (ADC2) and four (ADC4) b-value diffusion metrics. Concordance of the majority of implementations was excellent for both phantom ADC measures and in vivo ADC2, with relative biases <0.1% (ADC2) and <0.5% (phantom ADC4) but with higher deviations in ADC at the lowest phantom ADC values. In vivo ADC4 concordance was good, with typical biases of ±2% to 3% but higher for online maps. Multiple b-value ADC implementations were separated into two groups determined by the fitting algorithm. Intergroup mean ADC differences ranged from negligible for phantom data to 2.8% for ADC4 in vivo data. Some higher deviations were found for individual implementations and online parametric maps. Despite generally good concordance, implementation biases in ADC measures are sometimes significant and may be large enough to be of concern in multisite studies.