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Plasma dopa decarboxylase activity in treatment-resistantrecent-onset psychosis patients

机译:血浆多巴脱羧酶活性对治疗有抗性近期发作的精神病患者

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摘要

Treatment resistance (TR) in psychosis is a major clinical problem. A biomarker predicting TR against conventional antipsychotic drugs would be relevant, potentially reducing unnecessary delay to adequate treatment with clozapine. Dopa decarboxylase (DDC) activity in the striatum, measured with positron emission tomography, is elevated in responders, but not in treatment-resistant patients. Plasma DDC activity could be a surrogate marker for DDC brain activity, and thus a potential biomarker that could be used in daily clinical practice. Therefore, we determined plasma DDC activity in 40 male patients with recent-onset psychosis, of whom the majority had started treatment, whereby 21 turned out to be treatment responders and 19 treatment resistant during follow up. We observed no significant group differences. Furthermore, symptom severity was not associated with plasma DCC activity. We did observe a trend level difference in the distribution of plasma DDC activity across categories of medication, with subsequent post hoc analysis showing lower DDC activity in risperidone-using patients. This may suggest that risperidone could influence plasma DDC activity. Based on these results, plasma DDC activity does not appear to be a promising biomarker for TR in recent-onset psychosis patientswho are already receiving antipsychotic treatment.
机译:精神病的治疗抵抗力(TR)是主要的临床问题。预测抗常规抗精神病药的TR的生物标志物将是相关的,从而可能减少氯氮平适当治疗的不必要延误。用正电子发射断层扫描术测量的纹状体中的多巴脱羧酶(DDC)活性在应答者中升高,但在抗药性患者中却没有升高。血浆DDC活性可能是DDC脑活性的替代指标,因此可能在日常临床实践中使用。因此,我们确定了40例新近发作的精神病男性患者的血浆DDC活性,其中大多数已开始治疗,其中21例为治疗反应者,19例为治疗耐药。我们没有观察到明显的群体差异。此外,症状严重程度与血浆DCC活性无关。我们确实观察到了不同药物类别中血浆DDC活性分布的趋势水平差异,随后的事后分析显示,使用利培酮的患者的DDC活性较低。这可能表明利培酮可能影响血浆DDC活性。根据这些结果,血浆DDC活性似乎不是近期发作的精神病患者TR的有前途的生物标志物已经在接受抗精神病药物治疗的人。

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