| Literature DB >> 6333496 |
H D Burns, R F Dannals, B Langström, H T Ravert, S E Zemyan, T Duelfer, D F Wong, J J Frost, M J Kuhar, H N Wagner.
Abstract
Carbon-11-labeled 3-N-methylspiperone, a positron-emitting dopamine-receptor antagonist with potential for use in positron emission tomography studies of human neurotransmitter receptors, was synthesized from 11CO2 in 40 min, with a radiochemical yield of approximately 20-40%. The specific activity of the (3-N-[11C]methyl)-spiperone was determined by ultraviolet spectroscopy to be approximately 270 mCi/mumol at the end of synthesis. In in vitro binding experiments, the Ki for 3-N-methylspiperone was found to be approximately 250 pM (against H-3 spiperone). The brain-to-blood ratios in normal ICR mice were 2.8 or greater at the times studied, and the striatum-to-cerebellum ratio at 60 min after injection was 20:1.Entities:
Mesh:
Substances:
Year: 1984 PMID: 6333496
Source DB: PubMed Journal: J Nucl Med ISSN: 0161-5505 Impact factor: 10.057