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1. Effect of intermittent subchronic MK‐801 administration on dopamine synthesis capacity and responsiveness in the prefrontal cortex.

Author

Shibata, Kazuro, Enomoto, Kosuke, Tsutsumi, Takahiro, Muraoka, Hiroyuki, Fuwa, Tatsu, Kawano, Masahiko, Ishigooka, Jun, Inada, Ken, Nishimura, Katsuji, and Oshibuchi, Hidehiro

Subjects
KETAMINE, DOPAMINE, PREFRONTAL cortex, HIGH performance liquid chromatography, METHYL aspartate receptors, GLUTAMATE receptors, DOPAMINE antagonists
Abstract

Aim: The therapeutic potential of N‐methyl‐D‐aspartate glutamate receptor (NMDAR) antagonists, particularly ketamine, in mood disorders, is linked to their modulation of dopamine dynamics in the medial prefrontal cortex (mPFC). However, conflicting effects of distinct NMDAR antagonists, like ketamine and phencyclidine, on mPFC dopamine levels stem from variances in their receptor affinity profiles. This study investigates the impact of intermittent subchronic administration of an NMDAR antagonist on dopamine synthesis capacity and responsiveness within the mPFC, focusing on Dizocilpine (MK‐801), a highly selective NMDAR antagonist. Methods: In vivo microdialysis and high‐performance liquid chromatography assessed extracellular dopamine levels in the mPFC following subchronic MK‐801 treatment. Locomotor activity was measured using a computed video tracking system. Results: Intermittent subchronic MK‐801 administration, followed by a 24‐h withdrawal, preserved both dopamine synthesis capacity and responsiveness to MK‐801 challenge in the mPFC. However, altered locomotor activity was observed, deviating from previous findings indicating impaired dopamine synthesis and responsiveness in the mPFC with twice‐daily subchronic NMDAR antagonist treatment. Conclusion: These findings offer crucial biochemical insights into the diverse impacts of NMDAR antagonists on dopamine dynamics and the distinct therapeutic mechanisms associated with ketamine in depression treatment. However, further investigation is imperative to pinpoint potential inconsistencies stemming from variances in drug type, dosage, or administration frequency. [ABSTRACT FROM AUTHOR]

Published
2024
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4. In Vivo Screening of Illegal Drug

Author

Ogata, Akio, primary, Satoh, Kanako, additional, Fuwa, Tatsu, additional, Tanaka, Toyohito, additional, Nagasawa, Akemichi, additional, Yuzawa, Katsuhiro, additional, Yano, Norio, additional, Ando, Hiroshi, additional, Kubo, Yoshikazu, additional, Takahashi, Hiroshi, additional, Ohyama, Ken-ichi, additional, Miyazawa, Maki, additional, and Kojima, Takashi, additional

Published
2013
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5. Pael receptor is involved in dopamine metabolism in the nigrostriatal system

Author

Imai, Yuzuru, primary, Inoue, Haruhisa, additional, Kataoka, Ayane, additional, Hua-Qin, Wang, additional, Masuda, Masao, additional, Ikeda, Toshio, additional, Tsukita, Kayoko, additional, Soda, Mariko, additional, Kodama, Tohru, additional, Fuwa, Tatsu, additional, Honda, Yoshiko, additional, Kaneko, Satoshi, additional, Matsumoto, Sadayuki, additional, Wakamatsu, Kazumasa, additional, Ito, Shosuke, additional, Miura, Masami, additional, Aosaki, Toshihiko, additional, Itohara, Shigeyoshi, additional, and Takahashi, Ryosuke, additional

Published
2007
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28. Differential expression of cFos following administration of two tremorgenic agents

Author

Miwa, Hideto, Nishi, Katsunori, Fuwa, Tatsu, and Mizuno, Yoshikuni

Abstract

The regional distribution of c-Fos expression in the brain after the administration of two tremorgenic agents was studied. In both the harmaline- and oxotremorin-treated rats, c-Fos-positive neurons were extensively distributed in the basal ganglia nuclei and the cerebellum. Additionally, in the harmalinetreated rats, numerous c-Fos-positive neurons were also distributed throughout the inferior olivary nucleus. In the oxotremorine-treated rats, while the inferior olive was not involved, c-Fos was strongly expressed in the neurons of the reticular thalamic nucleus, possibly due to the muscarinic effects of oxotremorine. The present study revealed that the inferior olive is selectively activated in the harmaline-administered animals and that the basal ganglia are involved in both harmaline- and oxotremorine-induced tremors.

Published
2000

29. Injection of a GABA antagonist into the mesopontine reticular formation abolishes haloperidolinduced catalepsy in rats

Author

Miwa, Hideto, Fuwa, Tatsu, Yokochi, Masayuki, Nishi, Katsunori, and Mizuno, Yoshikuni

Abstract

THE pedunculopontine nucleus and its adjacent structure of the mesopontine reticular formation are known as a mesencephalic locomotor region, since either electrical or chemical stimulation of these regions induces locomotion in decerebrate animals. In parkinsonism, it is presumed that the pedunculopontine nucleus is under GABAergic overinhibition from the basal ganglia. To reveal the behavioural effects of GABAergic disinhibition of the mesopontine reticular formation in parkinsonism, picrotoxin, a GABAAantagonist, (5 or 10 ng/0.25 μl) or vehicle was injected unilaterally into the mesopontine reticular formation of rats via implanted cannulae after induction of catalepsy using haloperidol (1.5 mg kg−1, i.p.). Injection of the larger dose of picrotoxin, but not the smaller dose nor the vehicle, abolished the catalepsy with or without spontaneous locomotor activity. The present result suggests that the disinhibition of the brainstem output structures contributes to the recovery of mobility in the cataleptic state induced by blocking the dopaminergic transmission of the basal ganglia.

Published
1996

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