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A new 111in-bleomycin complex for tumor imaging: Preparation, stability, and distribution in glioma-bearing mice

✍ Scribed by De-Yan Hou; Hans Hoch; Gerald S. Johnston; K. C. Tsou; Alfred E. Jones; Raymond J. Farkas; Elizabeth E. Miller


Publisher
John Wiley and Sons
Year
1984
Tongue
English
Weight
895 KB
Volume
25
Category
Article
ISSN
0022-4790

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✦ Synopsis


Abstract

A new ^111^In‐bleomycin complex (^111^In‐BLMC) is here reported. Its radiochemical purity was 99% by thin‐layer chromatography (TLC) (Rf 0.65) and in 5% agarose gel electrophoresis in 0.02 M NaHCO~3~ it migrated toward the anode. Autoradiographs of TLC and gel electrophoresis plates showed no change on storage for 3 weeks. Urine and plasma from untreated or glioma‐bearing mice after injection of ^111^In‐BLMC were analyzed by TLC and gel electrophoresis. Results indicated stability in vivo, nonbinding to transferrin, affinity to viable tumor, and excretion faster than ^111^In‐BLM‐B~2~, ^111^In‐BLM, or ^57^Co‐BLM. Tissue distributions 24 hr after injection of radiopharmaceutical showed activity ratios of tumor to blood, muscle, and brain of 13.1, 12.4, and 81.6, respectively, which were significantly higher than those for previously prepared ^111^In‐BLM‐B~2~ or ^111^In‐BLM (except for brain, 0.05 < P < 0.1). The new ^111^In‐BLM complex may be useful in clinical imaging and for combining radionuclide radiotherapy and chemotherapy.


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A new tumor imaging agent-111In-bleomyci
✍ De-Yan Hou; Hans Hoch; Gerald S. Johnston; K. C. Tsou; Alfred E. Jones; Elizabet 📂 Article 📅 1984 🏛 John Wiley and Sons 🌐 English ⚖ 778 KB

## Abstract We have found a new ^111^In‐bleomycin complex (BLMC), which has high affinity to tumor, does not bind to transferrin and is stable in vivo. Distribution in animals bearing glioma, hepatoma, or mammary adenocarcinoma at 48 hours showed: the ratios of tumor to blood, brain, heart, lung, l