Building on recent work on psychophysiological deviance in two late-adolescent, psychometrically defined populations believed vulnerable to developing psychosis, the project will investigate cognitive abnormalities in these groups. The goals of the project are (1) to refine objective psychophysiological selection criteria for identifying vulnerable individuals; and (2) to evaluate a theory of the information processing abnormalities manifested by these individuals, preparatory to developing cognitively oriented preventive interventions targeted at these abnormalities. Cognitive tasks derived from normative information processing models will be completed by subjects chosen for vulnerability to psychosis, as well as by dysthymic and non-psychiatric controls. These tasks are selected especially to involve anticipatory processing of affective and non-affective stimuli. Extensive psychophysiological measurement during task performance will demonstrate contrasts between vulnerable and control subjects' handling of affective stimuli. Based on task-specific information processing models, these psychophysiological abnormalities will implicate specific cognitive differences in the vulnerable individuals. These studies will enhance the early diagnosis and primary prevention of psychotic disorders, by strengthening a relatively untapped and underdeveloped domain of assessment for identifying vulnerable individuals. Psychophysiological predictors are especially promising as an adjunct to traditional screening methods, since current psychophysiological functioning may more directly tap the biochemical abnormalities which are suspected in psychosis. Of particular interest are known psychophysiological differences between the two vulnerable populations under investigation. By determining the cognitive basis of and refining psychophysiological markers for these differences, individually tailored preventive interventions can be designed which address the specific difficulties and/or vulnerabilities of each population.

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH039628-05
Application #
3377525
Study Section
Psychopathology and Clinical Biology Research Review Committee (PCB)
Project Start
1986-02-01
Project End
1992-11-30
Budget Start
1991-02-01
Budget End
1991-11-30
Support Year
5
Fiscal Year
1991
Total Cost
Indirect Cost
Name
University of Illinois Urbana-Champaign
Department
Type
Schools of Arts and Sciences
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820
Deldin, Patricia; Keller, Jennifer; Casas, Brooks R et al. (2006) Normal N400 in mood disorders. Biol Psychol 71:74-9
Nitschke, Jack B; Heller, Wendy; Etienne, Marci A et al. (2004) Prefrontal cortex activity differentiates processes affecting memory in depression. Biol Psychol 67:125-43
Miller, G A; Chapman, J P (2001) Misunderstanding analysis of covariance. J Abnorm Psychol 110:40-8
Weber, T A; Kramer, A F; Miller, G A (1997) Selective processing of superimposed objects: an electrophysiological analysis of object-based attentional selection. Biol Psychol 45:159-82
Miller, G A (1996) How we think about cognition, emotion, and biology in psychopathology. Psychophysiology 33:615-28
Yee, C M; Miller, G A (1994) A dual-task analysis of resource allocation in dysthymia and anhedonia. J Abnorm Psychol 103:625-36
Deldin, P J; Duncan, C C; Miller, G A (1994) Season, gender, and P300. Biol Psychol 39:15-28
Giese-Davis, J E; Miller, G A; Knight, R A (1993) Memory template comparison processes in anhedonia and dysthymia. Psychophysiology 30:646-56
Klein, D N; Miller, G A (1993) Depressive personality in nonclinical subjects. Am J Psychiatry 150:1718-24
Yee, C M; Deldin, P J; Miller, G A (1992) Early stimulus processing in dysthymia and anhedonia. J Abnorm Psychol 101:230-3

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