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Vol.30 No.2, pp. 84-88

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  • Korean Journal of Biological Psychiatry
  • Volume 5(1); 1998
  • Article

Review

Korean Journal of Biological Psychiatry 1998;5(1):83-94. Published online: Jan, 1, 1998

Abstract PDF Full Text

Association of Schizophrenia with Pathological Aging:A Behavioral and Histological Study Using Animal Model

  • Jin-Sook Cheon, MD1;Byoung-Hoon Oh, MD2; and Hwan-Il Chang, MD3;
    1;Department of Neuropsychiatry, Kosin University, School of Medicine, Pusan, 2;Department of Neuropsychiatry, Yonsei University, College of Medicine, Seoul, 3;Department of Neuropsychiatry, Kyunghee University, Medical College, Seoul, Korea
Abstract

Objectives:Phencyclidine(PCP) or PCP-like substances such as ketamine have been known to rekindle the cognitive dysfunction in schizophrenia. The aims of this study were to identify whether PCP-like substances can produce cognitive deficit in schizophrenia, to discuss relation with aging process, and finally to speculate underlying neurochemical mecha-nisms by various drug responses.

Methods:In experiment I, radial maze tests were done in 24 Sprague-Dawley rats for 3 days to get baseline data. Being divided into 4 groups(6 rats respectively) of normal aged, normal adult controls, atropine-treated and ketamine-treated, the radial maze tests were repeated on every week for 6 weeks, and then the rats were sacrificed by intracardiac perfusion with phosphate-buffered 10% formaldehyde solution for histology. The brain specimen was stained with hematoxylin-eosin to count cells in the prefrontal cortex and hippocampus. In experiment II, radial maze tests were done for 48 rats before any drug treatment and only after ketamine administration. Thereafter, haloperidol, bromocriptine, clonidine, nimodipine, tacrine, valproic acid, naloxone and fluoxetine were intramuscularly injected on every other day in addition to ketamine. Radial maze tests were repeated on every week for 6 weeks, and then rats were prepared by the same procedure for histology.

Results:1) Reaction times of radial maze tests of atropine-treated rats were significantly prolonged than those of normal aged(p<0.05) or normal adult controls(p<0.05). Cell numbers of prefrontal cortex & hippocampus in ketamine-treated rats were significantly reduced than those in normal aged(p<0.05) or normal adult controls(p<0.005). 2) Reduced cell numbers by ketamine became significantly raised by tacrine administration in prefrontal cortex & hippocampus(p<0.05), while there were no significant changes on radial maze tests. Cell numbers also tended to be raised by nimodipine, fluoxetine and haloperidol administration.

Conclusions:In conclusion, the visuospatial memory disorders in ketamine-induced psychotic rats might be partly asso-ciated with aging process. Furthermore, the responses to the various drugs suggested cholinergic system might have an important role in the neurochemical mechanism of the cognitive dysfunction in ketamine-induced psychosis. Otherwise, calcium metabolism as well as serotonergic and dopaminergic systems seemed to be possibly related.

Keywords Ketamine;Visuospatial memory disorders;Aging;Radial maze tests;Prefrontal cortex;Acetylcholine.