CYP2D6 基因 1846G > A 多态性与急性酒精性幻觉症患者氟哌啶醇平衡浓度水平的关系。

Psychopharmacology bulletin Pub Date : 2023-12-04
A A Parkhomenko, M S Zastrozhin, VYu Skryabin, A E Petukhov, S A Pozdniakov, V A Ivanchenko, I A Zaytsev, I V Bure, P O Bochkov, K A Akmalova, V V Smirnov, E A Bryun, D A Sychev
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引用次数: 0

摘要

氟哌啶醇目前在成瘾学中用于治疗急性精神病,包括急性酒精性幻觉。在使用氟哌啶醇的同时,经常会出现药物不良反应(ADRs)。目的:该研究旨在评估 CYP2D6 基因 1846G > A 多态性与急性酒精性幻觉症患者氟哌啶醇平衡浓度水平的关系:研究对象为 100 名急性酒精性幻觉症男性患者(平均年龄为 41.4 ± 14.4 岁)。疗效采用 PANSS(阳性和阴性综合征量表)量表进行评估。治疗的安全性采用 UKU 副作用评定量表和 SAS(辛普森-安格斯锥体外系症状量表)量表进行评估。基因分型采用实时聚合酶链反应(Real-time PCR)进行。使用高效液相色谱-质谱法(HPLC-MS/MS)检测氟哌啶醇的平衡血浆浓度水平:结果:在疗效评估(PANSS评分的动态变化、GG基因型(-13.00%)、PANSS评分的动态变化、PANSS评分的动态变化)中没有发现有统计学意义的结果:GG基因型(-13.00 [-16.00; -16.00; -11.00]),GA基因型(-15.00 [-16.75; -13.00],P = 0.728)。安全性评估得分(UKU 评分动态变化)差异有统计学意义:GG基因型(8.00 [7.00; 10.00]),GA基因型(15.00 [9.25; 18.00],p < 0.001);SAS评分动态:GG基因型(11.00 [9.00; 14.00]),GA基因型(14.50 [12.00; 18.00],P <0.001)。药代动力学研究结果显示,两者之间存在显著的统计学差异:GG(3.13 [2.32; 3.95]),GA(3.89 [2.92; 5.26],p = 0.010)。因此,一项针对 100 名急性酒精性幻觉症患者的研究表明,CYP2D6 基因的 1846G > A 多态性(rs3892097)与氟哌啶醇治疗的安全性之间存在关联。我们还发现,GG 和 AG 基因型患者的氟哌啶醇平衡浓度水平存在显著的统计学差异:结论:与 GG 基因型患者相比,GA 基因型患者发生不良反应的风险更高。研究表明,CYP2D6 基因的 1846G > A 多态性(rs3892097)对氟哌啶醇的平衡浓度水平有显著的统计学影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Relationship of the 1846G > A Polymorphism of the CYP2D6 Gene to the Equilibrium Concentration Levels of Haloperidol in Patients with Acute Alcoholic Hallucinosis.

Haloperidol is currently used in addictology for the treatment of acute psychotic disorders, including acute alcoholic hallucinosis. The use of haloperidol is often accompanied by the occurrence of adverse drug reactions (ADRs). There is evidence that CYP2D6 isoenzyme is involved in the biotransformation of haloperidol.

Aim: The study aimed to evaluate the relationship of 1846G > A polymorphism of the CYP2D6 gene to the equilibrium concentration levels of haloperidol in patients with acute alcoholic hallucinosis.

Material and methods: The study was conducted on 100 male patients with acute alcoholic hallucinosis (mean age 41.4 ± 14.4 years). The efficacy profile was evaluated using the PANSS (Positive and Negative Syndrome Scale) scale. The safety of therapy was assessed using the UKU Side-Effect Rating Scale and the SAS (Simpson-Angus Scale for Extrapyramidal Symptoms) scale. Genotyping was performed using the real-time polymerase chain reaction (Real-time PCR). Equilibrium plasma concentration levels of haloperidol were investigated using the high-performance liquid chromatography with mass spectrometry (HPLC with MS/MS).

Results: No statistically significant results were obtained during the therapy efficacy assessment (dynamics of the PANSS score: GG genotype (-13.00 [-16.00; -16.00; -11.00]), GA genotype (-15.00 [-16.75; -13.00], p = 0.728). There was a statistically significant difference in safety assessment scores (dynamics of the UKU score: GG genotype (8.00 [7.00; 10.00]), GA genotype (15.00 [9.25; 18.00], p < 0.001); dynamics of the SAS score: GG genotype (11.00 [9.00; 14.00]), GA genotype (14.50 [12.00; 18.00], p < 0.001). The pharmacokinetic study results showed a statistically significant difference: GG (3.13 [2.32; 3.95]), GA (3.89 [2.92; 5.26], p = 0.010). Thus, a study conducted on a group of 100 patients with acute alcoholic hallucinosis demonstrated an association between the 1846G > A polymorphism of the CYP2D6 gene (rs3892097) and the safety profile of haloperidol therapy. We also revealed the presence of statistically significant difference in the equilibrium concentration levels of haloperidol in patients with the GG and AG genotypes.

Conclusion: It can be concluded that patients with the GA genotype have a higher risk of ADRs compared to patients carrying the GG genotype. It is shown that 1846G > A polymorphism of the CYP2D6 gene (rs3892097) has a statistically significant effect on the equilibrium concentration levels of haloperidol.

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