Abstract

In order to improve tracers for amino acid transport studies with SPET we have radioionated methylated tyrosines and compared their brain uptake and in vivo deiodination in mice. O-methylation not only leads to a higher lipophilicity and hence significantly higher brain uptake with a maximum of 5% dose/g for 3-[ 123I]iodo- O- methyl- l-α- methyltyrosine (OMIMT) but also significantly prevents in vivo deiodination. High n.c.a. radioiodination yields (⩾80%) are obtained for the activated aromatic compounds l-tyrosine and l-α-methyltyrosine using Iodo-gen tm in a heterogeneous aqueous system. Direct n.c.a. radioiodination of the less-activated O-methyl analogues has been achieved in reasonable yields (60%) with Iodo-gen tm in homogeneous TFA solutions containing about 10% of water.

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