Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane

Measurement of tumour and normal tissue perfusion in vivo in cancer patients will aid the clinical development of antiangiogenic and antivascular agents. We investigated the potential antiangiogenic effects of the drug razoxane by measuring the changes in parameters estimated from H(2)(15)O and C(15...

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Autores principales: Anderson, H, Yap, J T, Wells, P, Miller, M P, Propper, D, Price, P, Harris, A L
Formato: Texto
Lenguaje:English
Publicado: Nature Publishing Group 2003
Materias:
Clinical
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2394254/
https://www.ncbi.nlm.nih.gov/pubmed/12865914
http://dx.doi.org/10.1038/sj.bjc.6601105
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author Anderson, H
Yap, J T
Wells, P
Miller, M P
Propper, D
Price, P
Harris, A L
author_facet Anderson, H
Yap, J T
Wells, P
Miller, M P
Propper, D
Price, P
Harris, A L
author_sort Anderson, H
collection PubMed
description Measurement of tumour and normal tissue perfusion in vivo in cancer patients will aid the clinical development of antiangiogenic and antivascular agents. We investigated the potential antiangiogenic effects of the drug razoxane by measuring the changes in parameters estimated from H(2)(15)O and C(15)O positron emission tomography (PET) to indicate alterations in vascular physiology. The study comprised 12 patients with primary or metastatic renal tumours >3 cm in diameter enrolled in a Phase II clinical trial of oral razoxane. Perfusion, fractional volume of distribution of water (VD) and blood volume (BV) were measured in tumour and normal tissue before and 4–8 weeks after treatment with 125 mg twice-daily razoxane. Renal tumour perfusion was variable but lower than normal tissue: mean 0.87 ml min(−1) ml(−1) (range 0.33–1.67) compared to renal parenchyma: mean 1.65 ml min(−1) ml(−1) (range 1.16–2.88). In eight patients, where parallel measurements were made during the same scan session, renal tumour perfusion was significantly lower than in normal kidney (P=0.0027). There was no statistically significant relationship between pretreatment perfusion and tumour size (r=0.32, n=13). In six patients scanned before and after razoxane administration, there was no statistically significant change in tumour perfusion: mean perfusion pretreatment was 0.81 ml min(−1) ml(−1) (range 0.46–1.26) and perfusion post-treatment was 0.72 ml min(−1) ml(−1) (range 0.51–1.15, P=0.15). Tumour VD and BV did not change significantly following treatment: mean pretreatment VD=0.66 (range 0.50–0.87), post-treatment VD=0.71 (range 0.63–0.82, P=0.22); pretreatment BV=0.18 ml ml(−1) (range 0.10–0.25), post-treatment BV=0.167 ml ml(−1) (range 0.091–0.24, P=0.55). Tumour perfusion, VD and BV did not change significantly with tumour progression. This study has shown that H(2)(15)O and C(15)O PET provide useful in vivo physiological measurements, that even highly angiogenic renal cancers have poor perfusion compared to surrounding normal tissue, and that PET can provide valuable information on the in vivo biology of angiogenesis in man and can assess the effects of antiangiogenic therapy.
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spelling pubmed-23942542009-09-10 Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane Anderson, H Yap, J T Wells, P Miller, M P Propper, D Price, P Harris, A L Br J Cancer Clinical Measurement of tumour and normal tissue perfusion in vivo in cancer patients will aid the clinical development of antiangiogenic and antivascular agents. We investigated the potential antiangiogenic effects of the drug razoxane by measuring the changes in parameters estimated from H(2)(15)O and C(15)O positron emission tomography (PET) to indicate alterations in vascular physiology. The study comprised 12 patients with primary or metastatic renal tumours >3 cm in diameter enrolled in a Phase II clinical trial of oral razoxane. Perfusion, fractional volume of distribution of water (VD) and blood volume (BV) were measured in tumour and normal tissue before and 4–8 weeks after treatment with 125 mg twice-daily razoxane. Renal tumour perfusion was variable but lower than normal tissue: mean 0.87 ml min(−1) ml(−1) (range 0.33–1.67) compared to renal parenchyma: mean 1.65 ml min(−1) ml(−1) (range 1.16–2.88). In eight patients, where parallel measurements were made during the same scan session, renal tumour perfusion was significantly lower than in normal kidney (P=0.0027). There was no statistically significant relationship between pretreatment perfusion and tumour size (r=0.32, n=13). In six patients scanned before and after razoxane administration, there was no statistically significant change in tumour perfusion: mean perfusion pretreatment was 0.81 ml min(−1) ml(−1) (range 0.46–1.26) and perfusion post-treatment was 0.72 ml min(−1) ml(−1) (range 0.51–1.15, P=0.15). Tumour VD and BV did not change significantly following treatment: mean pretreatment VD=0.66 (range 0.50–0.87), post-treatment VD=0.71 (range 0.63–0.82, P=0.22); pretreatment BV=0.18 ml ml(−1) (range 0.10–0.25), post-treatment BV=0.167 ml ml(−1) (range 0.091–0.24, P=0.55). Tumour perfusion, VD and BV did not change significantly with tumour progression. This study has shown that H(2)(15)O and C(15)O PET provide useful in vivo physiological measurements, that even highly angiogenic renal cancers have poor perfusion compared to surrounding normal tissue, and that PET can provide valuable information on the in vivo biology of angiogenesis in man and can assess the effects of antiangiogenic therapy. Nature Publishing Group 2003-07-21 2003-07-15 /pmc/articles/PMC2394254/ /pubmed/12865914 http://dx.doi.org/10.1038/sj.bjc.6601105 Text en Copyright © 2003 Cancer Research UK https://creativecommons.org/licenses/by/4.0/This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material.If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit https://creativecommons.org/licenses/by/4.0/.
spellingShingle Clinical
Anderson, H
Yap, J T
Wells, P
Miller, M P
Propper, D
Price, P
Harris, A L
Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane
title Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane
title_full Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane
title_fullStr Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane
title_full_unstemmed Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane
title_short Measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase II clinical trial of razoxane
title_sort measurement of renal tumour and normal tissue perfusion using positron emission tomography in a phase ii clinical trial of razoxane
topic Clinical
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2394254/
https://www.ncbi.nlm.nih.gov/pubmed/12865914
http://dx.doi.org/10.1038/sj.bjc.6601105
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