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A validation of cognitive biomarkers for the early identification of cognitive enhancing agents in schizotypy: a three-center double-blind placebo-controlled study.

Koychev, Ivan; McMullen, Katrina; Lees, Jane; Dadhiwala, Rukiya; Grayson, Lois; Perry, Charlotte; Schmechtig, Anne; Walters, James; Craig, Kevin J; Dawson, Gerard R; Dourish, Colin T; Ettinger, Ulrich; Wilkinson, Lawrence; Williams, Steven; Deakin, John Francis William; Barkus, Emma

European neuropsychopharmacology : the journal of the European College of Neuropsychopharmacology. 2012;22(7):469-81.

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Abstract

A number of compounds aimed at improving cognition in schizophrenia have failed to demonstrate efficacy in Phase 2 clinical trials. Translational studies using biomarkers in surrogate populations, such as schizotypy, could be used to assess the efficacy of novel compounds. In this study, we aimed to validate the sensitivity and inter-site reliability of cognitive biomarkers (working memory (N-back), spatial working memory (SWM) and verbal fluency (VF) tasks) to detect the schizotypy phenotype and its reversal by psychotropic drugs. Healthy volunteers scoring high or average on a schizotypal personality measure (122 in each group) were randomized to receive a single dose of risperidone, amisulpride, nicotine or placebo in a double-blind, between-subject design. We found evidence for a poorer performance on N-back and VF tasks in the high schizotypy group, replicating previous research. This effect was counteracted by amisulpride on N-back: it improved working memory in high schizotypy group but impaired the controls. A similar pattern was seen in SWM and VF. We interpret this finding in the light of the dopamine enhancing action of amisulpride when given in low doses. In contrast, risperidone impaired both groups and nicotine had a beneficial effect for the low baseline performers only. These effects were consistent across sites. These data demonstrates the utility of biomarkers in detecting the effect of schizotypy and its reversal by drugs that enhance dopamine and cholinergic function. Studies using similar design could help the early assessment of potential of compounds designed to improve cognition in schizophrenia.

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Published date:
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ISSN:
Place of publication:
Netherlands
Volume:
22
Issue:
7
Pagination:
469-81
Digital Object Identifier:
10.1016/j.euroneuro.2011.10.005
Pubmed Identifier:
22137565
Pii Identifier:
S0924-977X(11)00268-9
Access state:
Active

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Record metadata

Manchester eScholar ID:
uk-ac-man-scw:253923
Created by:
Deakin, Bill
Created:
27th January, 2015, 15:51:24
Last modified by:
Deakin, Bill
Last modified:
27th January, 2015, 15:51:24

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