@article{oai:repo.qst.go.jp:00046149,
 author = {Toyohara, Jun and Nariai, Tadashi and Sakata, Muneyuki and Oda, Keiichi and Ishii, Kenji and Irie, Toshiaki and Saga, Tsuneo and Kubota, Kazuo and Ishiwata, Kiichi and 豊原 潤 and 成相 直 and 入江 俊章 and 佐賀 恒夫},
 issue = {8},
 journal = {Journal of Nuclear Medicine},
 month = {Aug},
 note = {Recently, we developed [methyl-11C]4'-thiothymidine (11C-4DST) as an in vivo cell proliferation marker. The present study was performed to determine the safety, distribution, radiation dosimetry, and initial brain tumor imaging of 11C-4DST in humans. Methods: Multiorgan biodistribution and radiation dosimetry of 11C-4DST were assessed in 3 healthy humans, who underwent 2-h whole-body PET scanning. Radiation dosimetry was estimated from the residence times of source organs using the OLINDA program. Six brain tumor patients underwent dynamic 11C-4DST scans with arterial blood sampling. These patients were also evaluated with 11C-methionine PET on the same day (n = 4) as, or 3 wk before (n = 2), 11C-4DST PET studies. Metabolites in plasma and urine samples were analyzed by high-performance liquid chromatography. Breakdown of the blood–brain barrier in tumor tissue was confirmed by gadolinium-enhanced T1-weighted MRI. Results: There were no serious adverse events in any subjects at any time during the study period. 11C-4DST PET demonstrated selective uptake in the bone marrow, which has a high rate of proliferation. In addition, high-level uptake was also seen in the liver. The highest absorbed organ dose was in the urinary bladder wall (17.6 muGy/MBq). The estimated effective dose for 11C-4DST was 4.2 muSv/MBq. 11C-4DST showed little uptake in normal brain tissues, resulting in low background activity for imaging of brain tumors. In contrast, 11C-4DST PET demonstrated rapid uptake in aggressive tumor masses, whereas no signal of 11C-4DST was seen in clinically stable disease in which 11C-methionine uptake was high. The distribution pattern of 11C-methionine in tumor regions was not always identical to that of 11C-4DST. Analysis of plasma samples by high-performance liquid chromatography indicated that more than 60% of the radioactivity was present as unchanged 11C-4DST at 20 min. Conclusion: The initial findings of the present study in a small group of patients indicated that 11C-4DST PET is feasible for imaging of brain tumors. Dosimetry and pharmacologic safety were acceptable at the dose required for adequate PET images.},
 pages = {1322--1328},
 title = {Whole-Body Distribution and Brain Tumor Imaging with 11C-4DST: a Pilot Study},
 volume = {52},
 year = {2011}
}