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Erschienen in: European Journal of Nuclear Medicine and Molecular Imaging 1/2004

01.01.2004 | Molecular Imaging

Iodine-124-labeled iodo-azomycin-galactoside imaging of tumor hypoxia in mice with serial microPET scanning

verfasst von: Pat Zanzonico, Joseph O’Donoghue, J Donald Chapman, Richard Schneider, Shangde Cai, Steven Larson, Bixiu Wen, Yuchun Chen, Ronald Finn, Shutian Ruan, Leo Gerweck, John Humm, Clifton Ling

Erschienen in: European Journal of Nuclear Medicine and Molecular Imaging | Ausgabe 1/2004

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Abstract

Tumor hypoxia, present in many human cancers, can lead to resistance to radiation and chemotherapy, is associated with a more aggressive tumor phenotype and is an independent prognostic factor of clinical outcome. It is therefore important to identify and localize tumor hypoxia in cancer patients. In the current study, serial microPET imaging was used to evaluate iodine-124-labeled iodo-azomycin-galactoside (124I-IAZG) (4.2-day physical half-life) as a hypoxia imaging agent in 17 MCa breast tumors and six FSaII fibrosarcomas implanted in mice. For comparison, another promising hypoxic-cell PET radiotracer, fluorine-18-labeled fluoro-misonidazole (18F-FMISO), was also imaged in the same tumor-bearing animals. Twelve animals were also imaged with 18F-labeled fluoro-deoxyglucose (18F-FDG). In addition, histological examination was performed, and direct measurement of tumor oxygenation status carried out with the Oxylite probe system. Two size groups were used, relatively well-oxygenated tumors in the range of 80–180 mg were designated as small, and those >300 mg and highly hypoxic, as large. Based on the data from 11 MCa and six FSaII tumors, both 124I-IAZG and 18F-FMISO images showed high tracer uptake in the large tumors. In 18F-FMISO images at 1, 3–4, and 6–8 h post-injection (p.i.), there was considerable whole-body background activity. In contrast, 124I-IAZG imaging was optimal when performed at 24–48 h p.i., when the whole-body background had dissipated considerably. As a result, the 124I-IAZG images at 24–48 h p.i. had higher tumor to whole-body activity contrast than the 18F-FMISO images at 3–6 h p.i. Region-of-interest analysis was performed as a function of time p.i. and indicated a tumor uptake of 5–10% (of total-body activity) for FMISO at 3–6 h p.i., and of ~17% for IAZG at 48 h p.i. This was corroborated by biodistribution data in that the tumor-to-normal tissue (T/N, normal tissues of blood, heart, lung, liver, spleen, kidney, intestine, and muscle) activity ratios of IAZG at 24 h p.i. was 1.5–2 times higher than those of FMISO at 3 h p.i., with the exception of stomach. Statistical analysis indicated that these differences in T/N ratios were significant. The small tumors were visualized in the 18F-FDG images, but not in the 124I-IAZG or 18F-FMISO images. This was perhaps due to the combined effect of a smaller tumor volume and a lower hypoxic fraction. Oxylite probe measurement indicated a lesser proportion of regions with pO2<2.5 mmHg in the small tumors (e.g., pO2 was <2.5 mmHg in 28% and 67% of the data in small and large FSaII tumors, respectively), and the biodistribution data showed lower uptake of the tracers in the small tumors than in the large tumors. In the first study of its kind, using serial microPET imaging in conjunction with biodistribution analysis and direct probe measurements of local pO2 to evaluate tumor hypoxia markers, we have provided data showing the potential of 124I-IAZG for hypoxia imaging.
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Metadaten
Titel
Iodine-124-labeled iodo-azomycin-galactoside imaging of tumor hypoxia in mice with serial microPET scanning
verfasst von
Pat Zanzonico
Joseph O’Donoghue
J Donald Chapman
Richard Schneider
Shangde Cai
Steven Larson
Bixiu Wen
Yuchun Chen
Ronald Finn
Shutian Ruan
Leo Gerweck
John Humm
Clifton Ling
Publikationsdatum
01.01.2004
Verlag
Springer-Verlag
Erschienen in
European Journal of Nuclear Medicine and Molecular Imaging / Ausgabe 1/2004
Print ISSN: 1619-7070
Elektronische ISSN: 1619-7089
DOI
https://doi.org/10.1007/s00259-003-1322-y

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