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

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 carcinom...

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Autores principales: Little, Ross A., Jamin, Yann, Boult, Jessica K. R., Naish, Josephine H., Watson, Yvonne, Cheung, Susan, Holliday, Katherine F., Lu, Huiqi, McHugh, Damien J., Irlam, Joely, West, Catharine M. L., Betts, Guy N., Ashton, Garry, Reynolds, Andrew R., Maddineni, Satish, Clarke, Noel W., Parker, Geoff J. M., Waterton, John C., Robinson, Simon P., O’Connor, James P. B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Radiological Society of North America 2018
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6122194/
https://www.ncbi.nlm.nih.gov/pubmed/29869970
http://dx.doi.org/10.1148/radiol.2018171531
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author Little, Ross A.
Jamin, Yann
Boult, Jessica K. R.
Naish, Josephine H.
Watson, Yvonne
Cheung, Susan
Holliday, Katherine F.
Lu, Huiqi
McHugh, Damien J.
Irlam, Joely
West, Catharine M. L.
Betts, Guy N.
Ashton, Garry
Reynolds, Andrew R.
Maddineni, Satish
Clarke, Noel W.
Parker, Geoff J. M.
Waterton, John C.
Robinson, Simon P.
O’Connor, James P. B.
author_facet Little, Ross A.
Jamin, Yann
Boult, Jessica K. R.
Naish, Josephine H.
Watson, Yvonne
Cheung, Susan
Holliday, Katherine F.
Lu, Huiqi
McHugh, Damien J.
Irlam, Joely
West, Catharine M. L.
Betts, Guy N.
Ashton, Garry
Reynolds, Andrew R.
Maddineni, Satish
Clarke, Noel W.
Parker, Geoff J. M.
Waterton, John C.
Robinson, Simon P.
O’Connor, James P. B.
author_sort Little, Ross A.
collection PubMed
description 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 under a CC BY 4.0 license. Online supplemental material is available for this article.
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spelling pubmed-61221942018-09-04 Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology Little, Ross A. Jamin, Yann Boult, Jessica K. R. Naish, Josephine H. Watson, Yvonne Cheung, Susan Holliday, Katherine F. Lu, Huiqi McHugh, Damien J. Irlam, Joely West, Catharine M. L. Betts, Guy N. Ashton, Garry Reynolds, Andrew R. Maddineni, Satish Clarke, Noel W. Parker, Geoff J. M. Waterton, John C. Robinson, Simon P. O’Connor, James P. B. Radiology Original Research 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 under a CC BY 4.0 license. Online supplemental material is available for this article. Radiological Society of North America 2018-09 2018-06-05 /pmc/articles/PMC6122194/ /pubmed/29869970 http://dx.doi.org/10.1148/radiol.2018171531 Text en http://creativecommons.org/licenses/by/4.0/ Published under a (http://creativecommons.org/licenses/by/4.0/) CC BY 4.0 license.
spellingShingle Original Research
Little, Ross A.
Jamin, Yann
Boult, Jessica K. R.
Naish, Josephine H.
Watson, Yvonne
Cheung, Susan
Holliday, Katherine F.
Lu, Huiqi
McHugh, Damien J.
Irlam, Joely
West, Catharine M. L.
Betts, Guy N.
Ashton, Garry
Reynolds, Andrew R.
Maddineni, Satish
Clarke, Noel W.
Parker, Geoff J. M.
Waterton, John C.
Robinson, Simon P.
O’Connor, James P. B.
Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology
title Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology
title_full Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology
title_fullStr Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology
title_full_unstemmed Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology
title_short Mapping Hypoxia in Renal Carcinoma with Oxygen-enhanced MRI: Comparison with Intrinsic Susceptibility MRI and Pathology
title_sort mapping hypoxia in renal carcinoma with oxygen-enhanced mri: comparison with intrinsic susceptibility mri and pathology
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6122194/
https://www.ncbi.nlm.nih.gov/pubmed/29869970
http://dx.doi.org/10.1148/radiol.2018171531
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