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Drug-Induced Dyskinesia, Part 2: Treatment of Tardive Dyskinesia.药物诱发的运动障碍,第 2 部分:迟发性运动障碍的治疗。
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Vesicular monoamine transporters: structure-function, pharmacology, and medicinal chemistry.囊泡单胺转运体:结构-功能、药理学和药物化学。
Med Res Rev. 2011 Jul;31(4):483-519. doi: 10.1002/med.20187. Epub 2010 Feb 4.

缬苯那嗪(NBI-98854)在患有迟发性运动障碍且诊断为精神分裂症或心境障碍的受试者中的长期安全性和耐受性。

Long-Term Safety and Tolerability of Valbenazine (NBI-98854) in Subjects with Tardive Dyskinesia and a Diagnosis of Schizophrenia or Mood Disorder.

作者信息

Josiassen Richard C, Kane John M, Liang Grace S, Burke Joshua, O'Brien Christopher F

机构信息

Dr. Josiassen, Translational Neuroscience, Conshohocken, PA; Dr. Kane, Hofstra Northwell School of Medicine, Hempstead, NY; Drs. Liang, Burke, O'Brien, Neurocrine Biosciences, Inc., San Diego, CA.

出版信息

Psychopharmacol Bull. 2017 Aug 1;47(3):61-68.

PMID:28839341
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5546552/
Abstract

BACKGROUND

The short-term safety profile of once-daily valbenazine (NBI-98854) has been evaluated in several double-blind, placebo-controlled (DBPC) trials in adults with tardive dyskinesia (TD) who had a diagnosis of schizophrenia/schizoaffective (SCHZ) disorder or mood disorder. Studies with longer treatment duration (up to 48 weeks) were conducted to evaluate the long-term safety of this novel drug in subjects with TD.

METHODS

The pooled long-term exposure (LTE) population included valbenazine-treated subjects from 3 studies: KINECT (NCT01688037: 6-week DBPC, 6-week open-label); KINECT 3 (NCT02274558: 6-week DBPC, 42-week blinded extension, 4-week drug-free follow-up); KINECT 4 (NCT02405091: 48-week open-label, 4-week drug-free follow-up). Safety assessments included adverse events (AEs), laboratory tests, vital signs, electrocardiograms (ECGs), and extrapyramidal symptom (EPS) scales. Psychiatric stability was monitored using the Positive and Negative Syndrome Scale (PANSS) and Calgary Depression Scale for Schizophrenia (CDSS) (SCHZ subgroup), as well as the Montgomery-Åsberg Depression Rating Scale (MADRS) and Young Mania Rating Scale (YMRS) (mood subgroup). All data were analyzed descriptively.

RESULTS

The LTE population included 430 subjects (KINECT, n = 46; KINECT 3, n = 220; KINECT 4, n = 164), 71.7% with SCHZ and 28.3% with a mood disorder; 85.5% were taking an antipsychotic (atypical only, 69.8%; typical only or typical + atypical, 15.7%). In the LTE population, treatment-emergent AEs (TEAEs) and discontinuations due to AEs were reported in 66.5% and 14.7% of subjects, respectively. The TEAE incidence was lower in the SCHZ subgroup (64.4%) than in the mood subgroup (71.9%). The 3 most common TEAEs in the SCHZ subgroup were urinary tract infection (UTI, 6.1%), headache (5.8%), and somnolence (5.2%). The 3 most common TEAEs in the mood subgroup were headache (12.4%), UTI (10.7%), and somnolence (9.1%). Mean score changes from baseline to end of treatment (Week 48) indicated that psychiatric stability was maintained in the SCHZ subgroup (PANSS Total, -3.4; PANSS Positive, -1.1; PANSS Negative, -0.1; PANSS General Psychopathology, -2.2; CDSS total, -0.4) and the mood subgroup (MADRS Total, 0.0; YMRS Total, -1.2). These scores remained generally stable during the 4-week drug-free follow-up periods. In the LTE population, mean changes in laboratory parameters, vital signs, ECG, and EPS scales were generally minimal and not clinically significant.

CONCLUSION

Valbenazine appeared to be well tolerated in adults with TD who received up to 48 weeks of treatment. In addition to long-term efficacy results (presented separately), these results suggest that valbenazine may be appropriate for the long-term management of TD regardless of underlying psychiatric diagnosis (SCHZ disorder or mood disorder).

摘要

背景

在数项针对患有迟发性运动障碍(TD)且诊断为精神分裂症/分裂情感性障碍(SCHZ)或心境障碍的成人患者的双盲、安慰剂对照(DBPC)试验中,已对每日一次服用的缬苯那嗪(NBI-98854)的短期安全性进行了评估。开展了治疗持续时间更长(长达48周)的研究,以评估这种新型药物在TD患者中的长期安全性。

方法

汇总的长期暴露(LTE)人群包括来自3项研究中接受缬苯那嗪治疗的受试者:KINECT(NCT01688037:6周双盲、6周开放标签);KINECT 3(NCT02274558:6周双盲、42周盲法延长期、4周停药后随访);KINECT 4(NCT02405091:48周开放标签、4周停药后随访)。安全性评估包括不良事件(AE)、实验室检查、生命体征、心电图(ECG)和锥体外系症状(EPS)量表。使用阳性和阴性症状量表(PANSS)以及精神分裂症卡尔加里抑郁量表(CDSS)(SCHZ亚组),以及蒙哥马利-Åsberg抑郁评定量表(MADRS)和杨氏躁狂评定量表(YMRS)(心境亚组)监测精神状态稳定性。所有数据均进行描述性分析。

结果

LTE人群包括430名受试者(KINECT,n =  46;KINECT 3,n = 220;KINECT 4,n = 164),71.7%患有SCHZ,28.3%患有心境障碍;85.5%正在服用抗精神病药物(仅非典型药物,69.8%;仅典型药物或典型药物+非典型药物,15.7%)。在LTE人群中,分别有66.5%和14.7%的受试者报告了治疗中出现的不良事件(TEAE)和因AE导致的停药情况。SCHZ亚组的TEAE发生率(64.4%)低于心境亚组(71.9%)。SCHZ亚组中3种最常见的TEAE为尿路感染(UTI,6.1%)、头痛(5.8%)和嗜睡(5.2%)。心境亚组中3种最常见的TEAE为头痛(12.4%)、UTI(10.7%)和嗜睡(9.1%)。从基线到治疗结束(第48周)的平均评分变化表明,SCHZ亚组(PANSS总分,-3.4;PANSS阳性,-1.1;PANSS阴性,-0.1;PANSS一般精神病理学,-2.2;CDSS总分,-0.4)和心境亚组(MADRS总分,0.0;YMRS总分,-1.2)的精神状态稳定性得以维持。在4周停药后随访期内,这些评分总体保持稳定。在LTE人群中,实验室参数、生命体征、ECG和EPS量表的平均变化通常极小,且无临床意义。

结论

在接受长达48周治疗的TD成人患者中,缬苯那嗪似乎耐受性良好。除了长期疗效结果(另行呈现)外,这些结果表明,无论潜在的精神疾病诊断(SCHZ障碍或心境障碍)如何,缬苯那嗪可能适用于TD的长期管理。