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AbstractAbstract
[en] Many animal models have been for studying neutrodegenerative diseases in humans. Among them, Parkinson's disease (PD) model in primates treated with 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) is expected to be valid and useful in the field of regenerative medicine. MPTP-treated monkeys demonstrate parkinsonian syndrome, such as tremor, dyskinesia, rigidity, immobility, caused by the degeneration of dopamine neurons at the nigrostriatal pathway. In this model, investigation of cognitive impairment that is one of the important aspects of PD could be possible. We evaluated the degeneration process of nigrostriatal dopamine neurons with positron emission tomography (PET) using unanesthetized MPTP-treated two cynomolgus monkeys (Macaca fascicularis). The tracers used were [11C]PE2I, [11C]DOPA, [11C]raclopride for monitoring dopamine transporter (DAT) densities, dopamine (DA) turnover, dopamine D2-receptor (D2R) densities, respectively. The gross behavioral observation was also performed referring to the criteria of the PD symptoms. The motor dysfunction was not clearly observed up to the cumulative doses of 3 mg/kg MPTP. This period was called 'asymptomatic period'. As a result of PET scans in the asymptomatic period, DAT densities and DA turnover had already decreased greatly, but D2R densities had not changed clearly. These findings suggest that PET imaging can delineate the dopaminergic dysfunction in vivo even in the asymptomatic period. In human study of PD, it is reported that parkinsonism is shown after great loss of dopaminergic neutrons as well as pre-synaptic dysfunction. MPTP-treated monkeys demonstrate the parkinsonian syndrome with the similar mechanism as human PD. It can be expected that PET study with MPTP-monkeys would provide important clues relevant to the underlying cause of PD and be useful for preclinical study of regenerative medicine in this disease. (author)
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Source
Tanada, Syuji (ed.); National Inst. of Radiological Sciences, Chiba (Japan); 48 p; Dec 2004; p. 16-18; 3. symposium of Research Center for Charged Particle Therapy on regenerative medicine and molecular imaging; Chiba, Chiba (Japan); 11-12 Dec 2003; Available from National Institute of Radiological Sciences, 4-9-1, Anagawa, Inage-ku, Chiba-shi, Chiba-ken 263-8555, Japan; 2 figs.
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Report
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Conference
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AMINES, ANIMAL CELLS, ANIMALS, AROMATICS, AUTONOMIC NERVOUS SYSTEM AGENTS, BETA DECAY RADIOISOTOPES, BETA-PLUS DECAY RADIOISOTOPES, BIOLOGICAL RECOVERY, CARBON ISOTOPES, CARDIOTONICS, CARDIOVASCULAR AGENTS, COMPUTERIZED TOMOGRAPHY, DIAGNOSTIC TECHNIQUES, DISEASES, DRUGS, EMISSION COMPUTED TOMOGRAPHY, EVEN-ODD NUCLEI, HYDROXY COMPOUNDS, ISOTOPE APPLICATIONS, ISOTOPES, LABELLED COMPOUNDS, LIGHT NUCLEI, MAMMALS, MATERIALS, MINUTES LIVING RADIOISOTOPES, NEUROREGULATORS, NUCLEI, ORGANIC COMPOUNDS, PHENOLS, POLYPHENOLS, PRIMATES, RADIOACTIVE MATERIALS, RADIOISOTOPES, SOMATIC CELLS, SYMPATHOMIMETICS, TOMOGRAPHY, VERTEBRATES
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