TY - JOUR
T1 - NMDA hypofunction in the posterior cingulate as a model for schizophrenia
T2 - An exploratory ketamine administration study in fMRI
AU - Northoff, Georg
AU - Richter, Andre
AU - Bermpohl, Felix
AU - Grimm, Simone
AU - Martin, Ernst
AU - Marcar, Valentine Leslie
AU - Wahl, Constance
AU - Hell, Daniel
AU - Boeker, Heinz
N1 - Funding Information:
The study was supported in part by a grant within the Postdoc-Programme of the German Academic Exchange Service (DAAD, D/02/46858) to F.B. and a Heisenberg grant from the German Research Foundation (DFG, 304/4-1) to G.N.
PY - 2005/1/1
Y1 - 2005/1/1
N2 - Based on animal data, NMDA receptor hypofunction has been suggested as a model for positive symptoms in schizophrenia. NMDA receptor hypofunction affects several corticolimbic brain regions, of which the posterior cingulate seems to be the most sensitive. However, empirical support for a crucial role of posterior cingulate NMDA hypofunction in the pathophysiology of positive symptoms is still missing in humans. We therefore conducted an fMRI study using the NMDA antagonist ketamine in healthy human subjects during episodic memory retrieval, which is supposed to activate the posterior cingulate. We investigated 16 healthy subjects which were assigned to either placebo (n=7; saline) or ketamine (n=9; 0.6 mg/kg/h) group in a double-blind study design. All subjects received their infusion while performing an episodic memory retrieval task in the scanner. Immediately after the fMRI session, psychopathological effects of ketamine were measured using the Altered States of Consciousness Questionnaire. The placebo group showed BOLD signal increases in the posterior and anterior cingulate during retrieval. Signal increases were significantly lower in the ketamine group. Lower signal increases in the posterior cingulate correlated significantly with positive (i.e. psychosis-like) symptoms induced by ketamine. The present study for the first time demonstrates a relationship between NMDA receptors, posterior cingulate and positive (i.e. psychosis-like) symptoms in humans. Confirming findings from animal studies, it supports the hypothesis of a pathophysiological role of NMDA receptor hypofunction in the posterior cingulate in schizophrenia.
AB - Based on animal data, NMDA receptor hypofunction has been suggested as a model for positive symptoms in schizophrenia. NMDA receptor hypofunction affects several corticolimbic brain regions, of which the posterior cingulate seems to be the most sensitive. However, empirical support for a crucial role of posterior cingulate NMDA hypofunction in the pathophysiology of positive symptoms is still missing in humans. We therefore conducted an fMRI study using the NMDA antagonist ketamine in healthy human subjects during episodic memory retrieval, which is supposed to activate the posterior cingulate. We investigated 16 healthy subjects which were assigned to either placebo (n=7; saline) or ketamine (n=9; 0.6 mg/kg/h) group in a double-blind study design. All subjects received their infusion while performing an episodic memory retrieval task in the scanner. Immediately after the fMRI session, psychopathological effects of ketamine were measured using the Altered States of Consciousness Questionnaire. The placebo group showed BOLD signal increases in the posterior and anterior cingulate during retrieval. Signal increases were significantly lower in the ketamine group. Lower signal increases in the posterior cingulate correlated significantly with positive (i.e. psychosis-like) symptoms induced by ketamine. The present study for the first time demonstrates a relationship between NMDA receptors, posterior cingulate and positive (i.e. psychosis-like) symptoms in humans. Confirming findings from animal studies, it supports the hypothesis of a pathophysiological role of NMDA receptor hypofunction in the posterior cingulate in schizophrenia.
KW - Episodic memory
KW - fMRI
KW - Ketamine
KW - NMDA receptors
KW - Positive symptoms
KW - Posterior cingulate
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U2 - 10.1016/j.schres.2004.04.009
DO - 10.1016/j.schres.2004.04.009
M3 - Article
C2 - 15560968
AN - SCOPUS:9244242541
SN - 0920-9964
VL - 72
SP - 235
EP - 248
JO - Schizophrenia Research
JF - Schizophrenia Research
IS - 2-3
ER -