Measuring liability for schizophrenia using optimized antisaccade stimulus parameters

JENNIFER E. McDOWELL; MARINA MYLES-WORSLEY; HILARY COON; WILLIAM BYERLEY; BRETT A. CLEMENTZ

doi:10.1017/S0048577299980836

Abstract

The ability to identify unaffected gene carriers within families may be crucial to the success of schizophrenia genetics studies. Data collected from three family samples (N = 365) demonstrated that poor antisaccade performance is an exceptionally promising indicator of liability for schizophrenia. A particular antisaccade task version provides large separations (5–6 sigma) between proband and normal groups. Poor antisaccade performance alone correctly identified 70% of patients in California, Utah, and Micronesia schizophrenia samples. Twenty-five to 50% of these patients' nonpsychotic first-degree relatives also had poor antisaccade performance, yielding risk ratios around 20:1 for simplex and 50:1 for multiplex schizophrenia families. Poor antisaccade performance is associated with dorsolateral prefrontal cortex pathology, suggesting that dysfunction of this circuitry also may predispose individuals to developing this disease.

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Measuring liability for schizophrenia using optimized antisaccade stimulus parameters

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