Kirsten Miller-Jaster scite author profile

Kirsten Miller-Jaster

4Publications

49Citation Statements Received

129Citation Statements Given

How they've been cited

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126

Affiliations

United States Army, National Institutes of Health, National Institutes of Health Clinical Center

Publications

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A computational pipeline for quantification of pulmonary infections in small animal models using serial PET-CT imaging

et al. 2013

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BackgroundInfectious diseases are the second leading cause of death worldwide. In order to better understand and treat them, an accurate evaluation using multi-modal imaging techniques for anatomical and functional characterizations is needed. For non-invasive imaging techniques such as computed tomography (CT), magnetic resonance imaging (MRI), and positron emission tomography (PET), there have been many engineering improvements that have significantly enhanced the resolution and contrast of the images, but there are still insufficient computational algorithms available for researchers to use when accurately quantifying imaging data from anatomical structures and functional biological processes. Since the development of such tools may potentially translate basic research into the clinic, this study focuses on the development of a quantitative and qualitative image analysis platform that provides a computational radiology perspective for pulmonary infections in small animal models. Specifically, we designed (a) a fast and robust automated and semi-automated image analysis platform and a quantification tool that can facilitate accurate diagnostic measurements of pulmonary lesions as well as volumetric measurements of anatomical structures, and incorporated (b) an image registration pipeline to our proposed framework for volumetric comparison of serial scans. This is an important investigational tool for small animal infectious disease models that can help advance researchers’ understanding of infectious diseases.MethodsWe tested the utility of our proposed methodology by using sequentially acquired CT and PET images of rabbit, ferret, and mouse models with respiratory infections of Mycobacterium tuberculosis (TB), H1N1 flu virus, and an aerosolized respiratory pathogen (necrotic TB) for a total of 92, 44, and 24 scans for the respective studies with half of the scans from CT and the other half from PET. Institutional Administrative Panel on Laboratory Animal Care approvals were obtained prior to conducting this research. First, the proposed computational framework registered PET and CT images to provide spatial correspondences between images. Second, the lungs from the CT scans were segmented using an interactive region growing (IRG) segmentation algorithm with mathematical morphology operations to avoid false positive (FP) uptake in PET images. Finally, we segmented significant radiotracer uptake from the PET images in lung regions determined from CT and computed metabolic volumes of the significant uptake. All segmentation processes were compared with expert radiologists’ delineations (ground truths). Metabolic and gross volume of lesions were automatically computed with the segmentation processes using PET and CT images, and percentage changes in those volumes over time were calculated. (Continued on next page)(Continued from previous page) Standardized uptake value (SUV) analysis from PET images was conducted as a complementary quantitative metric for disease severity assessment. Thus, severity and extent of p...

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Predicting Future Morphological Changes of Lesions from Radiotracer Uptake in 18F-FDG-PET Images

et al. 2013

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We introduce a novel computational framework to enable automated identification of texture and shape features of lesions on 18F-FDG-PET images through a graph-based image segmentation method. The proposed framework predicts future morphological changes of lesions with high accuracy. The presented methodology has several benefits over conventional qualitative and semi-quantitative methods, due to its fully quantitative nature and high accuracy in each step of (i) detection, (ii) segmentation, and (iii) feature extraction. To evaluate our proposed computational framework, thirty patients received 2 18F-FDG-PET scans (60 scans total), at two different time points. Metastatic papillary renal cell carcinoma, cerebellar hemongioblastoma, non-small cell lung cancer, neurofibroma, lymphomatoid granulomatosis, lung neoplasm, neuroendocrine tumor, soft tissue thoracic mass, nonnecrotizing granulomatous inflammation, renal cell carcinoma with papillary and cystic features, diffuse large B-cell lymphoma, metastatic alveolar soft part sarcoma, and small cell lung cancer were included in this analysis. The radiotracer accumulation in patients' scans was automatically detected and segmented by the proposed segmentation algorithm. Delineated regions were used to extract shape and textural features, with the proposed adaptive feature extraction framework, as well as standardized uptake values (SUV) of uptake regions, to conduct a broad quantitative analysis. Evaluation of segmentation results indicates that our proposed segmentation algorithm has a mean dice similarity coefficient of 85.75±1.75%. We found that 28 of 68 extracted imaging features were correlated well with SUVmax (p<0.05), and some of the textural features (such as entropy and maximum probability) were superior in predicting morphological changes of radiotracer uptake regions longitudinally, compared to single intensity feature such as SUVmax. We also found that integrating textural features with SUV measurements significantly improves the prediction accuracy of morphological changes (Spearman correlation coefficient = 0.8715, p<2e-16).

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Automatic quantification of Tree-in-Bud patterns from CT scans

Bağcı

Miller-Jaster

Yao³

et al. 2012

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In this paper, we present a fully automatic method to quantify Tree-in-Bud (TIB) patterns for respiratory tract infections. The proposed quantification method is based on our previous effort to detect and track TIB patterns with a computer assisted detection (CAD) system [9]. In addition to accurately identifying TIB on CT, quantifying TIB is important for measuring the volume of affected lung as a potantial marker of disease severity. This quantification can be challenging due to the complex shape of TIB and high intensity variation contributing mixed features. Our proposed quantification method is based on a local scale concept such that TIB regions detected via the CAD system are quantified adaptively, and volume percentages of the quantified regions are compared to visual scoring of participating radiologists. We conducted the experiments with a data set of 94 chest CTs (laboratory confirmed 39 viral bronchiolitis caused by human parainfluenza (HPIV), 34 nontuberculous mycobacterial (NTM), and 21 normal control). Experimental results show that the proposed quantification system is well suited to the CAD system for detecting TIB patterns. Correlations of observer-CAD agreements are reported as (R2 = 0.824, p < 0.01) and (R2 = 0.801, p < 0.01) for HPIV and NTM cases, respectively.

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Hydroxyurea Use for Sickle Cell Anemia Patients is Underutilized Even Within a Universal Health Care System

Miller-Jaster

Susi²,

Nylund³

et al. 2021

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