精神分裂症患者皮下注射 TV-46000 的长期安全性和耐受性研究:3期随机双盲临床试验。

IF 7.4 2区 医学 Q1 CLINICAL NEUROLOGY
CNS drugs Pub Date : 2024-08-01 Epub Date: 2024-07-02 DOI:10.1007/s40263-024-01102-2
John M Kane, Roy Eshet, Eran Harary, Orna Tohami, Anna Elgart, Helena Knebel, Nir Sharon, Mark Suett, Kelli R Franzenburg, Glen L Davis, Christoph U Correll
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引用次数: 0

摘要

背景:TV-46000是一种利培酮长效皮下抗精神病药(LASCA)制剂,已获美国食品药品管理局批准用于治疗成人精神分裂症。在利培酮皮下缓释剂(RISE)3 期随机双盲研究中,与安慰剂相比,每月一次(q1m)和每两个月一次(q2m)的 TV-46000 能显著延长即将复发的时间[5.0 倍(q1m)和 2.7 倍(q2m)]。这项TV-46000皮下注射人体安全性评估(SHINE)的3期随机双盲研究旨在评估TV-46000在精神分裂症患者中的长期安全性、耐受性和暴露情况:完成 RISE 而未复发(滚动)或新招募(从头开始)的患者有资格参加 SHINE 研究。患者最初使用利培酮口服药物稳定治疗12周(完成RISE的患者为转期患者,新招募的患者为SHINE患者)。在SHINE研究中,新患者队列中的患者和在RISE研究中接受安慰剂治疗的患者按1:1比例随机接受TV-46000 q1m或q2m治疗,疗程长达56周。SHINE的主要终点是报告的不良事件(AEs)频率;事件发生率[ER;每100患者年(PYs)的事件发生率]由患者根据一般询问计算得出:共有 336 名患者随机接受了 SHINE 治疗[TV-46000 q1m,n = 174;TV-46000 q2m,n = 162;其中,新患者,n = 109;滚转患者,n = 227(n = 172 名患者接受治疗,n = 55 名患者接受安慰剂治疗)]。共对 334 名患者进行了安全性评估[q1m,n = 172(PY = 97.8);q2m,n = 162(PY = 104.5)]。出现≥1次AE和≥1次治疗相关AE的患者(ER)比例分别为:TV-46000 q1m为37%(180.0)和21%(84.9),TV-46000 q2m为46%(157.9)和20%(70.8)。与治疗相关的常见不良反应[两组中均≥3%;患者比例(ER)]为注射部位疼痛[q1m,5%(24.5);q2m,4%(22.0)]和注射部位结节[q1m,2%(9.2);q2m,6%(12.4)]。TV-46000 q1m和TV-46000 q2m出现严重AEs的患者比例分别为5%和7%;总体上报告的严重AEs≥2例的患者为精神分裂症恶化[q1m,n = 1(< 1%;ER,1.02); q2m, n = 2 (1%; ER, 1.91)] 和高血糖 [q1m, n = 1 (< 1%; ER, 1.02); q2m, n = 1 (< 1%; ER, 0.96)]。在报告的三例死亡病例中,没有一例与治疗有关。总体而言,有8名患者因AE停止了治疗。与之前未接受过TV-46000治疗的患者相比,从TV-46000治疗中转入治疗的患者(新转入和安慰剂转入)的AEs发生率相似或略低。大多数与注射部位反应有关的不良反应都很轻微,没有患者出现严重反应:这项长期安全性研究的结果进一步证实了 TV-46000 q1m 和 q2m 具有良好的安全性,这与利培酮的其他制剂以及之前的 TV-46000 研究结果一致:注册:ClinicalTrials.gov,NCT03893825;2019年3月27日。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Long-Term Safety and Tolerability Study of TV-46000 for Subcutaneous Use in Patients with Schizophrenia: A Phase 3, Randomized, Double-Blinded Clinical Trial.

A Long-Term Safety and Tolerability Study of TV-46000 for Subcutaneous Use in Patients with Schizophrenia: A Phase 3, Randomized, Double-Blinded Clinical Trial.

Background: TV-46000 is a long-acting subcutaneous antipsychotic (LASCA) formulation of risperidone that is approved by the United States Food and Drug Administration for the treatment of schizophrenia in adults. In the phase 3, randomized, double-blind RIsperidone Subcutaneous Extended-release (RISE) study, TV-46000 once monthly (q1m) and once every 2 months (q2m) significantly prolonged time to impending relapse compared with placebo [5.0-fold (q1m) and 2.7-fold (q2m)]. This phase 3, randomized, double-blind Safety in Humans of TV-46000 subcutaneous INjection Evaluation (SHINE) study was designed to evaluate the long-term safety, tolerability, and exposure of TV-46000 in schizophrenia.

Methods: Patients who completed RISE without relapse (rollover) or who were newly recruited (de novo) were eligible for the SHINE study. Patients were initially stabilized on oral risperidone for 12 weeks (completed in RISE for rollover, or in SHINE for de novo). Patients in the de novo cohort and patients who received placebo in RISE were randomized 1:1 in SHINE to receive TV-46000 q1m or q2m for up to 56 weeks. Primary endpoint for SHINE was frequency of reported adverse events (AEs); event rates [ER; events per 100 patient-years (PYs)] were calculated for each AE by patients upon general questioning.

Results: Overall, 336 patients were randomized in SHINE [TV-46000 q1m, n = 174; TV-46000 q2m, n = 162; of these, de novo, n = 109 and rollover, n = 227 (n = 172 patients were treated and n = 55 received placebo)]. A total of 334 patients were evaluated for safety [q1m, n = 172 (PY = 97.8); q2m, n = 162 (PY = 104.5)]. Proportions of patients (ER) with ≥ 1 AE and ≥ 1 treatment-related AE were 37% (180.0) and 21% (84.9) for TV-46000 q1m and 46% (157.9) and 20% (70.8) for TV-46000 q2m, respectively. Frequent treatment-related AEs [≥ 3% of patients in either group; proportion of patients (ER)] were injection site pain [q1m, 5% (24.5); q2m, 4% (22.0)] and injection site nodule [q1m, 2% (9.2); q2m, 6% (12.4)]. The proportions of patients with serious AEs was 5% for TV-46000 q1m and 7% for TV-46000 q2m; serious AEs reported for ≥ 2 patients overall were worsening schizophrenia [q1m, n = 1 (< 1%; ER, 1.02); q2m, n = 2 (1%; ER, 1.91)] and hyperglycemia [q1m, n = 1 (< 1%; ER, 1.02); q2m, n = 1 (< 1%; ER, 0.96)]. Of three reported deaths, none were related to treatment. Overall, eight patients discontinued treatment because of AEs. Similar or somewhat lower rates of AEs were reported for patients who rolled over from TV-46000 treatment compared with those who had no prior TV-46000 treatment (de novo and placebo rollover). Most AEs related to injection site reactions were mild; no patient had a severe reaction.

Conclusion: Results from this long-term safety study add to the favorable safety profiles of TV-46000 q1m and q2m, consistent with other formulations of risperidone and previous studies with TV-46000.

Registration: ClinicalTrials.gov, NCT03893825; 27 March 2019.

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来源期刊
CNS drugs
CNS drugs 医学-精神病学
CiteScore
12.00
自引率
3.30%
发文量
82
审稿时长
6-12 weeks
期刊介绍: CNS Drugs promotes rational pharmacotherapy within the disciplines of clinical psychiatry and neurology. The Journal includes: - Overviews of contentious or emerging issues. - Comprehensive narrative reviews that provide an authoritative source of information on pharmacological approaches to managing neurological and psychiatric illnesses. - Systematic reviews that collate empirical evidence to answer a specific research question, using explicit, systematic methods as outlined by the PRISMA statement. - Adis Drug Reviews of the properties and place in therapy of both newer and established drugs in neurology and psychiatry. - Original research articles reporting the results of well-designed studies with a strong link to clinical practice, such as clinical pharmacodynamic and pharmacokinetic studies, clinical trials, meta-analyses, outcomes research, and pharmacoeconomic and pharmacoepidemiological studies. Additional digital features (including animated abstracts, video abstracts, slide decks, audio slides, instructional videos, infographics, podcasts and animations) can be published with articles; these are designed to increase the visibility, readership and educational value of the journal’s content. In addition, articles published in CNS Drugs may be accompanied by plain language summaries to assist readers who have some knowledge of, but not in-depth expertise in, the area to understand important medical advances.
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