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  • An odor-specific threshold deficit implicates abnormal cAMP signaling in youths at clinical risk for psychosis.

An odor-specific threshold deficit implicates abnormal cAMP signaling in youths at clinical risk for psychosis.

Schizophrenia research (2012-04-28)
Vidyulata Kamath, Paul J Moberg, Monica E Calkins, Karin Borgmann-Winter, Catherine G Conroy, Raquel E Gur, Christian G Kohler, Bruce I Turetsky
摘要

While olfactory deficits have been reported in schizophrenia and youths at-risk for psychosis, few studies have linked these deficits to current pathophysiological models of the illness. There is evidence that disrupted cyclic adenosine 3',5'-monophosphate (cAMP) signaling may contribute to schizophrenia pathology. As cAMP mediates olfactory signal transduction, the degree to which this disruption could manifest in olfactory impairment was ascertained. Odor-detection thresholds to two odorants that differ in the degree to which they activate intracellular cAMP were assessed in clinical risk and low-risk participants. Birhinal assessments of odor-detection threshold sensitivity to lyral and citralva were acquired in youths experiencing prodromal symptoms (n=17) and controls at low risk for developing psychosis (n=15). Citralva and lyral are odorants that differ in cAMP activation; citralva is a strong cAMP activator and lyral is a weak cAMP activator. The overall group-by-odor interaction was statistically significant. At-risk youths showed significantly reduced odor detection thresholds for lyral, but showed intact detection thresholds for citralva. This odor-specific threshold deficit was uncorrelated with deficits in odor identification or discrimination, which were also present. ROC curve analysis revealed that olfactory performance correctly classified at-risk and low-risk youths with greater than 97% accuracy. This study extends prior findings of an odor-specific hyposmia implicating cAMP-mediated signal transduction in schizophrenia and unaffected first-degree relatives to include youths at clinical risk for developing the disorder. These results suggest that dysregulation of cAMP signaling may be present during the psychosis prodrome.

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Sigma-Aldrich
4-(4-羟基-4-甲基戊基)-3-环己烯-1-甲醛, mixture of isomers, ≥97.0% (GC)