1. p-Fluorophenylglycine in the urine of baboons treated with HPTP, the tetrahydropyridine analog of haloperidol
- Author
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Lodewyk J. Mienie, Jeffrey R. Bloomquist, Stefanus J. Steyn, Neal Castagnoli, Jacobus J. Bergh, and Cornelis J. Van der Schyf
- Subjects
Male ,medicine.medical_specialty ,Dopamine ,Glycine ,Oxidative phosphorylation ,Urine ,Tardive dyskinesia ,General Biochemistry, Genetics and Molecular Biology ,Mice ,Internal medicine ,biology.animal ,medicine ,Haloperidol ,Animals ,Humans ,General Pharmacology, Toxicology and Pharmaceutics ,chemistry.chemical_classification ,biology ,Chemistry ,Neurotoxicity ,General Medicine ,medicine.disease ,In vitro ,Amino acid ,Endocrinology ,Propionates ,Oxidation-Reduction ,Antipsychotic Agents ,Papio ,Baboon ,medicine.drug - Abstract
We report the presence of p -fluorophenylglycine ( p -FPG) in the urine of six baboons treated with HPTP, the tetrahydropyridine dehydration product of haloperidol (HP). Oxidative N-dealkylation, the major metabolic pathway of HP, gives rise to 3-(4-fluorobenzoyl)propionic acid ( p -FBPA). Subsequent β-oxidation of p -FBPA produces p -fluorophenylacetic acid ( p -FPA). The presence of p -FPA argues for the formation also of p -fluorophenylglyoxylic acid ( p -FPGA) derived from β-oxidation of p -FBPA. Plasma aminotransferases should convert p -FPGA to p -FPG. The presence of p -FPG in these animals suggest the presence of phenylglycine aminotransferases in the baboon and possibly also in other primates, including the human. Reports by other authors found that treatment with α-phenylglycine (α-PG), an “unnatural” amino acid, leads to striatal dopamine (DA) depletion in rabbits — an effect explained on the basis of α-PG competing with DA for the neuronal vesicular storage sites. We performed in vitro DA release assays in mouse striatal synaptosomal preparations but found that neither α-PG nor p -FPG released any DA. It therefore remains unclear whether p -FPG may be a contributing factor to neurologic side-effects such as tardive dyskinesia (TD) found in patients after long-term HP treatment.
- Published
- 1999
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