4.3 Article

Animal-specific positioning molds for registration of repeat imaging studies: comparative microPET imaging of F18-labeled fluoro-deoxyglucose and fluoro-misonidazole in rodent tumors

Journal

NUCLEAR MEDICINE AND BIOLOGY
Volume 33, Issue 1, Pages 65-70

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.nucmedbio.2005.07.011

Keywords

image registration; hypoxia imaging; small-animal imaging; FDG; FMiso

Funding

  1. NCI NIH HHS [P50 CA96439-06, R01 CA84596, R24 CA83084, P30 CA08748] Funding Source: Medline
  2. NATIONAL CANCER INSTITUTE [R01CA084596, P30CA008748, R24CA083084] Funding Source: NIH RePORTER

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Introduction: Comparative imaging of multiple radiotracers in the same animal can be invaluable in elucidating and validating their respective mechanisms of localization. Comparative imaging of PET tracers, particularly in small animals, is problematic, however: such tracers must be administered and imaged separately because simultaneously imaged positron emitters cannot be separated based on energy discrimination. Objective: As part Of Our ongoing development of hypoxia imaging radiotracers, the intratumoral distributions of sequentially administered F18-fluoro-deoxyglucose (FDG) and the hypoxia tracer F18-fluoromisonidazole (FMiso) were compared in rats by registered microPET imaging with positioning of each animal in a custom-fabricated whole-body mold. Methods: Nude rats with a hindlimb R3327-AT anaplastic rat prostate tumor xenograft and a hindlimb FaDu human squamous cell carcinoma (each up to 20x20x30 mm in size) were studied. Rapid-Foam (Soule Medical, Lutz, FL) was used to fabricate animal-specific molds for immobilization and reproducible positioning. Each rat was injected via the tail vein with similar to 33 MBq (900 mu Ci) of FDG and imaged in its mold at 1 h postinjection (pi) on the microPET. The next day, each rat was injected with similar to 22 MBq (600 mu Ci) of FMiso and positioned and imaged in its mold at similar to 2 h pi. Custom-manufactured germanium-68 rods (10 mu Ci each, 1 x 10 mm) were reproducibly positioned in the mold as fiduciary markers. Results: The registered microPET images unambiguously demonstrated grossly similar though not identical distributions of FDG and FMiso in the tumors-a high-activity rim surrounding a lower-activity core. There were subtle but possibly significant differences in the intratumoral distributions of FDG and FMiso, however. These may not have been discerned without careful image registration. Conclusion: Animal-specific molds are inexpensive and straightforward to fabricate and use for registration (+/- 1 to 2 mm) of sequential PET images and may aid image interpretation. (c) 2006 Elsevier Inc. All rights reserved.

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