Terbinafine and risperidone drug interaction contributing to clinical changes in a forensic psychiatric patient.

Jamie Reynolds, Nicole Gramlich
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Abstract

Risperidone is a second generation "atypical" antipsychotic that exhibits its clinical effects through a combined effort of risperidone and its active metabolite, 9-hydroxyrisperidone (9-OHR), otherwise known as paliperidone. Risperidone is hepatically metabolized by the cytochrome P450 2D6 (CYP2D6) enzyme into 9-OHR. Significant interference with the metabolism of risperidone may lead to clinical consequences for patients via alterations in the ratio of the parent compound and active metabolite. This patient case reports 1 example of how a drug interaction could contribute to delayed response to a medication increase after psychiatric decompensation. A forensic psychiatric patient was transitioned from oral risperidone to risperidone microspheres long-acting injectable and had worsening of symptoms, necessitating an increased dose of the injection. This increase in symptoms may have been prolonged by addition of a CYP2D6 inhibitor, terbinafine. The changes in clinical symptoms correlate with medication concentrations that were drawn before terbinafine was started, during terbinafine therapy, and after terbinafine was discontinued.

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特比萘芬和利培酮药物相互作用对法医精神病患者临床变化的影响。
利培酮是第二代“非典型”抗精神病药物,其临床效果是通过利培酮及其活性代谢物9-羟基利培酮(9-OHR)的共同作用而显现的,也被称为帕利培酮。利培酮经细胞色素P450 2D6 (CYP2D6)酶肝脏代谢为9-OHR。对利培酮代谢的显著干扰可能通过改变母体化合物和活性代谢物的比例导致患者的临床后果。本病例报告了一个药物相互作用如何导致精神失代偿后药物增加反应延迟的例子。一名法医精神病患者从口服利培酮过渡到长效注射利培酮微球,症状恶化,需要增加注射剂量。这种症状的增加可能因添加CYP2D6抑制剂特比萘芬而延长。临床症状的变化与特比萘芬开始使用前、特比萘芬治疗期间和特比萘芬停药后的药物浓度有关。
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