Computerized detection of noncalcified plaques in coronary CT angiography: Evaluation of topological soft gradient prescreening method and luminal analysis

Peer Reviewedhttp://deepblue.lib.umich.edu/bitstream/2027.42/135084/1/mp5958.pd

Imaging Biomarkers of Pulmonary Structure and Function

Asthma and chronic obstructive pulmonary disease (COPD) are characterized by airflow limitations resulting from airway obstruction and/or tissue destruction. The diagnosis and monitoring of these pulmonary diseases is primarily performed using spirometry, specifically the forced expiratory volume in one second (FEV1), which measures global airflow obstruction and provides no regional information of the different underlying disease pathologies. The limitations of spirometry and current therapies for lung disease patients have motivated the development of pulmonary imaging approaches, such as computed tomography (CT) and magnetic resonance imaging (MRI). Inhaled hyperpolarized noble gas MRI, specifically using helium-3 (3He) and xenon-129 (129Xe) gases, provides a way to quantify pulmonary ventilation by visualizing lung regions accessed by gas during a breath-hold, and alternatively, regions that are not accessed - coined “ventilation defects.” Despite the strong foundation and many advantages hyperpolarized 3He MRI has to offer research and patient care, clinical translation has been inhibited in part due to the cost and need for specialized equipment, including multinuclear-MR hardware and polarizers, and personnel. Accordingly, our objective was to develop and evaluate imaging biomarkers of pulmonary structure and function using MRI and CT without the use of exogenous contrast agents or specialized equipment. First, we developed and compared CT parametric response maps (PRM) with 3He MR ventilation images in measuring gas-trapping and emphysema in ex-smokers with and without COPD. We observed that in mild-moderate COPD, 3He MR ventilation abnormalities were related to PRM gas-trapping whereas in severe COPD, ventilation abnormalities correlated with both PRM gas-trapping and PRM emphysema. We then developed and compared pulmonary ventilation abnormalities derived from Fourier decomposition of free-breathing proton (1H) MRI (FDMRI) with 3He MRI in subjects with COPD and bronchiectasis. This work demonstrated that FDMRI and 3He MRI ventilation defects were strongly related in COPD, but not in bronchiectasis subjects. In COPD only, FDMRI ventilation defects were spatially related with 3He MRI ventilation defects and emphysema. Based on the FDMRI biomarkers developed in patients with COPD and bronchiectasis, we then evaluated ventilation heterogeneity in patients with severe asthma, both pre- and post-salbutamol as well as post-methacholine challenge, using FDMRI and 3He MRI. FDMRI free-breathing ventilation abnormalities were correlated with but under-estimated 3He MRI static ventilation defects. Finally, based on the previously developed free-breathing MRI approach, we developed a whole-lung free-breathing pulmonary 1H MRI technique to measure regional specific-ventilation and evaluated both asthmatics and healthy volunteers. These measurements not only provided similar information as specific-ventilation measured using plethysmography, but also information about regional ventilation defects that were correlated with 3He MRI ventilation abnormalities. These results demonstrated that whole-lung free-breathing 1H MRI biomarker of specific-ventilation may reflect ventilation heterogeneity and/or gas-trapping in asthma. These important findings indicate that imaging biomarkers of pulmonary structure and function using MRI and CT have the potential to regionally reveal the different pathologies in COPD and asthma without the use of exogenous contrast agents. The development and validation of these clinically meaningful imaging biomarkers are critically required to accelerate pulmonary imaging translation from the research workbench to being a part of the clinical workflow, with the overall goal to improve patient outcomes

Morphologic evaluation of ruptured abdominal aortic aneurysm by 3D modeling

This thesis was created in Word and converted to PDF using Mac OS X 10.7.5 Quartz PDFContext.Abdominal aortic aneurysm (AAA) is defined as a dilatation of the abdominal aorta exceeding the normal diameter by more than 50%. The standard and widely used approach to assess AAA size is by measuring the maximal diameter (Dmax). Currently, the main predictors of rupture risk are the Dmax, sex, and the expansion rate of the aneurysm. Yet, Dmax has some limitations. AAAs of vastly different shapes may have the same maximal diameter. Dmax lacks sensitivity for rupture risk, especially among smaller AAAs. Thus, there is a need to evaluate the susceptibility of a given AAA to rupture on a patient-specific basis. We present the design concept and workflow of the AAA segmentation software developed at our institution. We describe the previous validation steps in which we evaluated the reproducibility of manual Dmax, compared software Dmax against manual Dmax, validated reproducibility of software Dmax and volume in cross-sectional and longitudinal studies for detection of AAA growth, and evaluated the reproducibility of software measurements in unenhanced computed tomographic angiography (CTA) and in the presence of stent-graft. In order to define new geometric features associated with rupture, we performed a case-control study in which we compared 63 cases with ruptured or symptomatic AAA and 94 controls with asymptomatic AAA. Univariate logistic regression analysis revealed 14 geometric indices associated with AAA rupture. In the multivariate logistic regression analysis, adjusting for Dmax and sex, the AAA with a higher bulge location and higher mean averaged surface area were associated with AAA rupture. Our preliminary results suggest that incorporating geometrical indices obtained by segmentation of CT shows a trend toward improvement of the classification accuracy of AAA with high rupture risk at CT over a traditional model based on Dmax and sex alone. Larger longitudinal studies are needed to verify the validity of the proposed model. Addition of flow and biomechanical simulations should be investigated to improve rupture risk prediction based on AAA modeling.Un anévrysme de l'aorte abdominale (AAA) est défini par une dilatation de plus de 50% par rapport au diamètre normal. La méthode standard et largement répandue pour mesurer la dimension d'un AAA consiste à mesurer le diamètre maximal (Dmax). Présentement, les principaux prédicteurs de risque de rupture sont le Dmax, le sexe et le taux d'expansion d'un anévrysme. Toutefois, le Dmax a certaines limitations. Des AAAs de formes très différentes peuvent avoir le même diamètre maximal. Le Dmax manque de sensibilité pour détecter le risque de rupture, en particulier pour les petits anévrysmes. Par conséquent, il y a un besoin d'évaluer de manière spécifique et individuelle la susceptibilité de rupture d'un AAA. Nous présentons le concept et le flux de travail d'un logiciel de segmentation des AAAs développé à notre institution. Nous décrivons les étapes antérieures de validation: évaluation de la reproductibilité du Dmax manuel, comparaison de Dmax par logiciel avec Dmax manuel, validation de la reproductibilité du Dmax et volume par logiciel dans des études transversale et longitudinale pour la détection de croissance et évaluation de la reproductibilité de mesures sur angiographie par tomodensitométrie et en présence d'endoprothèse. En vue d’identifier de nouveaux paramètres géométrique associés avec le risque de rupture, nous avons réalisé une étude cas-témoin comparant 63 cas avec AAA rompu ou symptomatique et 94 contrôles avec AAA asymptomatique. Une analyse de régression logistique univariée a identifié 14 indices géométriques associés avec une rupture de AAA. Dans l'analyse de régression logistique multivariée, en ajustant pour le Dmax et le sexe, les AAA avec un bombement plus haut situé et une surface moyenne plus élevée étaient associés à une rupture. Nos résultats préliminaires suggèrent que l'inclusion d'indices géométriques obtenus par segmentation de tomodensitométrie tend à améliorer la classification de AAA avec un risque de rupture par rapport à un modèle traditionnel seulement basé sur le Dmax et le sexe. De plus larges études longitudinales sont requises pour vérifier la validité du modèle proposé. Des simulations de flux et biomécaniques devraient être envisagées pour améliorer la prédiction du risque de rupture basée sur la modélisation d'anévrysmes