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11 results on '"Holliday, Katherine"'

1. Oxygen-enhanced MRI in cancer

Author

Holliday, Katherine Frances, Naish, Josephine, and Parker, Geoffrey

Subjects
616.99
Abstract

Tumour hypoxia is linked to reduced treatment sensitivity and poor outcome. Oxygen-enhanced MRI (OE-MRI) is a novel technique with the potential to non-invasively image hypoxia. It involves the measurement of MR relaxation rate changes caused by changes in oxygenation within blood and tissue. This thesis is focused on the development of OE-MRI and its clinical application in tumours. Two imaging sequences were optimised and then investigated for accuracy and precision in measuring oxygen enhanced R1 changes. Following that, R1, R2* and blood flow were measured during air and oxygen breathing in healthy kidneys. This study included the implementation of model-driven registration for inversion prepared OE-MRI images. Next, a biophysical model was used to simulate expected ΔR1 in tumour tissue during hyperoxia for a range of underlying physiological conditions. Finally, OE-MRI was applied alongside BOLD and DCE-MRI in clinical studies in renal and cervical tumours. It was shown that a dynamic inversion-prepared HASTE sequence in combination with a baseline T1 map offered the most precise measure of oxygen-enhanced ΔR1. No consistent significant change was found in either T1, R2* or blood flow when using static measures, but significant changes in R1 were found by using dynamicT1-weighted signal. Image registration had variable effect on dynamic signal curves, but reduced errors in T1 calculations. Modelling showed that differences in ΔR1 are mainly caused by the interplay between blood flow, oxygen consumption and capillary length. Finally, clinical studies demonstrated the feasibility of OE-MRI in tumours. The work in this thesis represents an improvement of OE-MRI methodology and offers a new insight into how results from OE-MRI relate to both underlying tumour physiology and other imaging modalities.

Published
2014

3. Mapping hypoxia in renal carcinoma with oxygen-enhanced MRI: comparison with intrinsic susceptibility MRI and pathology

Author

Little, Ross, Jamin, Yann, Boult, Jessica K R, Naish, Josephine, Watson, Yvonne, Cheung, Susan, Holliday, Katherine, Lu, Huiqi, Mchugh, Damien, Irlam, Joely, West, Catharine, Betts, Guy, Ashton, Garry, Reynolds, Andrew R., Maddineni, Satish, Clarke, Noel W, Parker, Geoff JM, Waterton, John, Robinson, Simon P., and O'Connor, James

Subjects
ResearchInstitutes_Networks_Beacons/MICRA, Manchester Institute for Collaborative Research on Ageing, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc
Abstract

Intrinsic susceptibility imaging and immunohistochemistry analysis were used to validate a combined endpoint of oxygen enhancement plus MR-derived perfusion as a biomarker of tumor hypoxia in mouse and patient studies. Purpose To cross-validate T1-weighted oxygen-enhanced (OE) MRI measurements of tumor hypoxia with intrinsic susceptibility MRI measurements and to demonstrate the feasibility of translation of the technique for patients. Materials and Methods Preclinical studies in nine 786–0-R renal cell carcinoma (RCC) xenografts and prospective clinical studies in eight patients with RCC were performed. Longitudinal relaxation rate changes (∆R1) after 100% oxygen inhalation were quantified, reflecting the paramagnetic effect on tissue protons because of the presence of molecular oxygen. Native transverse relaxation rate (R2*) and oxygen-induced R2* change (∆R2*) were measured, reflecting presence of deoxygenated hemoglobin molecules. Median and voxel-wise values of ∆R1 were compared with values of R2* and ∆R2*. Tumor regions with dynamic contrast agent–enhanced MRI perfusion, refractory to signal change at OE MRI (referred to as perfused Oxy-R), were distinguished from perfused oxygen-enhancing (perfused Oxy-E) and nonperfused regions. R2* and ∆R2* values in each tumor subregion were compared by using one-way analysis of variance. Results Tumor-wise and voxel-wise ∆R1 and ∆R2* comparisons did not show correlative relationships. In xenografts, parcellation analysis revealed that perfused Oxy-R regions had faster native R2* (102.4 sec–1 vs 81.7 sec–1) and greater negative ∆R2* (−22.9 sec–1 vs −5.4 sec–1), compared with perfused Oxy-E and nonperfused subregions (all P < .001), respectively. Similar findings were present in human tumors (P < .001). Further, perfused Oxy-R helped identify tumor hypoxia, measured at pathologic analysis, in both xenografts (P = .002) and human tumors (P = .003). Conclusion Intrinsic susceptibility biomarkers provide cross validation of the OE MRI biomarker perfused Oxy-R. Consistent relationship to pathologic analyses was found in xenografts and human tumors, demonstrating biomarker translation.

Published
2022

4. Noninvasive tumor hypoxia measurement using magnetic resonance imaging in murine U87 glioma xenografts and in patients with glioblastoma

Author

Linnik, Inna V., Scott, Marietta L. J., Holliday, Katherine F., Woodhouse, Neil, Waterton, John C., O'Connor, James P. B., Barjat, Hervé, Liess, Carsten, Ulloa, Jose, Young, Helen, Dive, Caroline, Hodgkinson, Cassandra L., Ward, Tim, Roberts, Darren, Mills, Samantha J., Thompson, Gerard, Buonaccorsi, Giovanni A., Cheung, Susan, Jackson, Alan, Naish, Josephine H., and Parker, Geoff J.M.

Published
2014
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7. Evaluation of dynamic contrast-enhanced MRI biomarkers for stratified cancer medicine: How do permeability and perfusion vary between human tumours?

Author

Little, Ross, Barjat, Hervé, Hare, Jennifer I., Jenner, Mary, Watson, Yvonne, Cheung, Susan, Holliday, Katherine, Zhang, Weijuan, O'Connor, James, Barry, Simon T, Puri, Sanyogitta, Parker, Geoff JM, and Waterton, John

Subjects
Imaging biomarkers, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc, Drug delivery, Solid tumors, personalised medicine, Dynamic contrast enhanced MRI, enhanced permeability and retention
Published
2018

8. Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology

Author

Little, Ross A., primary, Jamin, Yann, additional, Boult, Jessica K. R., additional, Naish, Josephine H., additional, Watson, Yvonne, additional, Cheung, Susan, additional, Holliday, Katherine F., additional, Lu, Huiqi, additional, McHugh, Damien J., additional, Irlam, Joely, additional, West, Catharine M. L., additional, Betts, Guy N., additional, Ashton, Garry, additional, Reynolds, Andrew R., additional, Maddineni, Satish, additional, Clarke, Noel W., additional, Parker, Geoff J. M., additional, Waterton, John C., additional, Robinson, Simon P., additional, and O’Connor, James P. B., additional

Published
2018
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9. Growth of human-milk fed and formula-fed infants with cystic fibrosis

Author

Holliday, Katherine E., Allen, Jane R., Waters, Donna L., Gruca, Margie A., Thompson, Susan M., and Gaskin, Kevin J.

Subjects
Growth -- Diet therapy, Cystic fibrosis -- Health aspects, Infant formulas -- Health aspects, Breast milk -- Health aspects, Health
Abstract

Cystic fibrosis (CF) is a disease characterized by pancreatic insufficiency that afflicts newborns and is fatal in many cases. When a timely diagnosis of CF is made, the infant may be given the necessary pancreatic enzymes to ensure proper growth, but the effect of feeding human milk or formula on the growth of these infants is unknown. A group of 65 infants with CF were divided into either the human milk-fed (41 infants) or the formula-fed group (24 infants). Birth weight and length measurements were obtained and subsequent measurements of weight and height were recorded at 3, 6, 12, 18 and 24 months. There was no significant difference in standardized height or weight measurements between the two groups from birth to 24 months. In addition, no distinction in growth patterns between pancreatic sufficient and nonsufficient infants in either group could be made. It appears that infants with CF who are fed human milk are as likely to grow as fast as infants with CF who are fed formula. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

10. Noninvasive tumor hypoxia measurement using magnetic resonance imaging in murine U87 glioma xenografts and in patients with glioblastoma

Author

Linnik, Inna V., primary, Scott, Marietta L. J., additional, Holliday, Katherine F., additional, Woodhouse, Neil, additional, Waterton, John C., additional, O'Connor, James P. B., additional, Barjat, Hervé, additional, Liess, Carsten, additional, Ulloa, Jose, additional, Young, Helen, additional, Dive, Caroline, additional, Hodgkinson, Cassandra L., additional, Ward, Tim, additional, Roberts, Darren, additional, Mills, Samantha J., additional, Thompson, Gerard, additional, Buonaccorsi, Giovanni A., additional, Cheung, Susan, additional, Jackson, Alan, additional, Naish, Josephine H., additional, and Parker, Geoff J.M., additional

Published
2013
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