Safety and Tolerability of Starting Aripiprazole Lauroxil With Aripiprazole Lauroxil NanoCrystal Dispersion in 1 Day Followed by Aripiprazole Lauroxil Every 2 Months Using Paliperidone Palmitate Monthly as an Active Control in Patients With Schizophrenia: A Post Hoc Analysis of a Randomized Controlled Trial.

IF 4.5 2区 医学 Q1 PSYCHIATRY Journal of Clinical Psychiatry Pub Date : 2024-02-28 DOI:10.4088/JCP.23m15095
Leslie Citrome, Sergey Yagoda, Ilda Bidollari, Meihua Wang
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Abstract

Background: Aripiprazole lauroxil (AL) 1064 mg every 2 months following initiation using the AL NanoCrystal Dispersion formulation (ALNCD) plus 30-mg oral aripiprazole was efficacious and well tolerated in a 25-week, randomized, double-blind phase 3 trial in adults with acute schizophrenia. This post hoc analysis further characterized the safety of AL 1064 mg administered every 2 months and that of active control paliperidone palmitate (PP) 156 mg monthly based on occurrence, timing, and severity of adverse events (AEs) associated with antipsychotic medications.

Methods: This study was conducted between November 2017 and March 2019. AL or PP was initiated during an inpatient stay of ≥ 2 weeks with transition to outpatient treatment thereafter. Rates of AEs of clinical interest, including injection site reactions (ISRs), motor AEs, sedation, hypotension, prolactin level increase, weight gain, and suicidal ideation/behavior, were summarized through weeks 4, 9, and 25 for each treatment.

Results: Of 200 patients who received ≥ 1 dose of study treatment, 99 (49.5%) completed the study (AL, 57%; PP, 43%). Mean (SD) baseline Positive and Negative Syndrome Scale total scores were 94.1 (9.04) and 94.6 (8.41) in the AL and PP treatment groups, respectively. AEs were reported by 69/99 (70%) patients administered AL and 72/101 (71%) administered PP; most AEs were mild or moderate in severity. ISRs (AL, 18.2%; PP, 26.7%) occurred primarily on days 1 and 8. All akathisia/restlessness AEs (AL, 10.1%; PP, 11.9%) occurred during the first 4 weeks; <10% of patients (either treatment) experienced hypotension, sedation, or suicidal ideation/behavior events. Weight gain of ≥ 7% from baseline occurred in 9.3% of AL- and 23.8% of PP-treated patients. Median prolactin concentrations changed by -4.60 and -3.55 ng/mL among AL-treated males and females, respectively, and did not exceed 2 times normal levels in any AL-treated patients. In PP-treated patients, changes were 21.20 and 80.40 ng/mL and concentrations exceeded 2 times normal in 38% and 88% of males and females, respectively.

Conclusions: No new early- or late-emerging safety concerns were observed through 25 weeks of treatment with AL 1064 mg every 2 months following initiation using ALNCD plus 30-mg oral aripiprazole. Results were consistent with known safety profiles of AL and PP and support the safety of AL 1064 mg every 2 months initiated using ALNCD plus 30-mg oral aripiprazole.

Trial Registration: ClinicalTrials.gov identifier: NCT03345979.

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精神分裂症患者在一天内开始使用阿立哌唑纳米结晶分散剂,随后每两个月使用一次阿立哌唑,并每月使用帕利哌酮棕榈酸酯作为活性对照的安全性和耐受性:随机对照试验的事后分析》。
背景:在对急性精神分裂症成人患者进行的一项为期25周的随机双盲3期试验中,在使用阿立哌唑纳米晶体分散制剂(ALNCD)加30毫克口服阿立哌唑开始治疗后,每2个月服用一次阿立哌唑月桂昔酯(AL)1064毫克,疗效显著且耐受性良好。这项事后分析根据与抗精神病药物相关的不良事件(AEs)的发生、时间和严重程度,进一步确定了每2个月给药一次的AL 1064毫克和每月给药一次的活性对照帕利哌酮棕榈酸酯(PP)156毫克的安全性:本研究于2017年11月至2019年3月期间进行。在住院≥2周期间开始使用AL或PP,之后转为门诊治疗。总结了每种治疗方法在第4周、第9周和第25周的临床相关AEs发生率,包括注射部位反应(ISRs)、运动AEs、镇静、低血压、催乳素水平升高、体重增加和自杀意念/行为:在接受了≥1个剂量研究治疗的200名患者中,99人(49.5%)完成了研究(AL,57%;PP,43%)。AL和PP治疗组基线阳性和阴性综合量表总分的平均值(标度)分别为94.1(9.04)和94.6(8.41)。69/99(70%)名接受 AL 治疗的患者和 72/101(71%)名接受 PP 治疗的患者报告了不良反应;大多数不良反应的严重程度为轻度或中度。ISR(AL,18.2%;PP,26.7%)主要发生在第 1 天和第 8 天。所有阿卡西尼症/躁动 AEs(AL,10.1%;PP,11.9%)均发生在最初的 4 周内;结论:没有新的早发或晚发 AEs:在使用ALNCD加30毫克口服阿立哌唑开始每2个月一次的AL 1064毫克治疗25周后,未观察到新的早期或晚期安全性问题。结果与已知的AL和PP的安全性特征一致,支持使用ALNCD加30毫克口服阿立哌唑开始每2个月服用AL 1064毫克的安全性:试验注册:ClinicalTrials.gov identifier:NCT03345979。
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来源期刊
Journal of Clinical Psychiatry
Journal of Clinical Psychiatry 医学-精神病学
CiteScore
7.40
自引率
1.90%
发文量
0
审稿时长
3-8 weeks
期刊介绍: For over 75 years, The Journal of Clinical Psychiatry has been a leading source of peer-reviewed articles offering the latest information on mental health topics to psychiatrists and other medical professionals.The Journal of Clinical Psychiatry is the leading psychiatric resource for clinical information and covers disorders including depression, bipolar disorder, schizophrenia, anxiety, addiction, posttraumatic stress disorder, and attention-deficit/hyperactivity disorder while exploring the newest advances in diagnosis and treatment.
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