美国精神分裂症患者使用毒蕈碱受体激动剂 KarXT(沙诺美林-曲司匹林)的疗效和安全性(EMERGENT-2):随机、双盲、安慰剂对照、灵活剂量的第 3 期试验结果

Inder Kaul, Sharon Sawchak, Christoph U Correll, Rishi Kakar, Alan Breier, Haiyuan Zhu, Andrew C Miller, Steven M Paul, Stephen K Brannan
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Beginning on day 8, KarXT dosing was flexible with an optional increase to 125 mg xanomeline and 30 mg trospium twice per day and the option to return to 100 mg xanomeline and 20 mg trospium based on tolerability. The primary endpoint was change from baseline to week 5 in PANSS total score. Efficacy analyses used the modified intention-to-treat population (all randomly assigned participants who received at least one trial medication dose and had at least one post-baseline PANSS assessment). </span>Least squares mean change from baseline, SE, and least squares mean difference between the KarXT and placebo groups at week 5, along with the 95% CI and two-sided p values were calculated for the primary and secondary continuous efficacy endpoints. Safety analyses included all participants receiving at least one trial medication dose and used descriptive statistics. 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引用次数: 0

摘要

精神分裂症患者迫切需要具有新机制的新疗法。Xanomeline是一种双重M1和m4偏好毒蕈碱受体激动剂,不阻断D2多巴胺受体,与目前所有批准的精神分裂症治疗方法不同。xanomeline- trospium (KarXT)将xanomeline与外周限制性毒蕈碱受体拮抗剂trospium chloride联合使用,目的是改善与外周毒蕈碱受体相关的xanomeline相关不良事件。emergency -2试验旨在评估KarXT对精神分裂症急性精神病患者的疗效和安全性。semergent -2是一项随机、双盲、安慰剂对照、灵活剂量、5周、住院、精神分裂症患者的3期临床试验。参与者是年龄在18-65岁之间的成年人,被诊断为精神分裂症,最近精神状况恶化,需要住院治疗,阳性和阴性综合征量表(PANSS)得分为80或更高,临床总体印象-严重程度得分为4或更高。参与者从美国22个住院部招募,并随机分配(1:1)到KarXT或安慰剂,每天两次。随机分配到KarXT的参与者在前2天每天两次接受50毫克xanomeline和20毫克trospium,然后在第3-7天每天两次接受100毫克xanomeline和20毫克trospium。从第8天开始,KarXT的剂量是灵活的,可选择每天两次增加到125 mg xanomeline和30 mg trospium,并可根据耐受性选择返回到100 mg xanomeline和20 mg trospium。主要终点是从基线到第5周PANSS总分的变化。疗效分析使用改良的意向治疗人群(所有随机分配的参与者接受至少一个试验药物剂量,并至少进行一次基线后PANSS评估)。计算第5周KarXT组和安慰剂组的基线最小二乘平均变化、SE和最小二乘平均差异,以及主要和次要连续疗效终点的95% CI和双侧p值。安全性分析包括接受至少一种试验药物剂量的所有参与者,并使用描述性统计。该试验已在ClinicalTrials.gov注册(NCT04659161)。从2020年12月16日到2022年4月13日,在407名接受筛查的患者中,252名符合入组标准的参与者被随机分配到KarXT (n=126)或安慰剂(n=126)组。基线PANSS总分为98·3分(KarXT;N =126)和97.9(安慰剂;n = 125)。该试验达到了主要终点,从基线到第5周,PANSS总分的平均变化有利于KarXT(- 21.2分,SE 1.7分),而安慰剂(- 11.6分,SE 1.6分;最小二乘均差-9·6;95% CI为- 13.9 ~ - 5.2;p< 0.0001, Cohen's d效应值= 0.61)。所有次要终点也得到满足,KarXT优于安慰剂(p< 0.05)。与安慰剂相比,KarXT最常见的不良事件是便秘(27例[21%]vs 13例[10%])、消化不良(24例[19%]vs 10例[8%])、头痛(17例[14%]vs 15例[12%])、恶心(24例[19%]vs 7例[6%])、呕吐(18例[14%]vs 1例[1%])、高血压(12例[10%]vs 1例[1%])、头晕(11例[9%]vs 4例[3%])、胃食管反流病(8例[6%]vs 0例[0%])和腹泻(7例[6%]vs 4例[3%])。治疗后出现的锥体外系运动症状不良事件发生率(KarXT, 0 [0%] vs安慰剂,0[0%])、静坐症(1 [1%]vs 1[1%])、体重增加(0 [0%]vs 1[1%])和嗜睡(6 [5%]vs 5[4%])在KarXT组和安慰剂组之间相似,不良事件相关的停药率(9 [7%]vs 7[6%])也相似。在emergency -2试验中,KarXT可有效减轻阳性和阴性症状,并且通常耐受性良好。这些结果支持KarXT代表了一种新的有效且耐受性良好的抗精神病药物的潜力,这种药物基于激活毒蕈碱受体,而不是目前所有抗精神病药物的D2多巴胺受体阻断机制。其他试验的结果,包括相同的急诊-3试验和52周的开放标签急诊-4和急诊-5试验,将提供关于KarXT治疗精神分裂症患者的有效性和安全性的额外信息。FundingKaruna疗法。
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Efficacy and safety of the muscarinic receptor agonist KarXT (xanomeline–trospium) in schizophrenia (EMERGENT-2) in the USA: results from a randomised, double-blind, placebo-controlled, flexible-dose phase 3 trial

Background

New treatments with new mechanisms are urgently needed for people with schizophrenia. Xanomeline is a dual M1 and M4-preferring muscarinic receptor agonist that does not block D2 dopamine receptors, unlike all currently approved treatments for schizophrenia. Xanomeline–trospium (KarXT) combines xanomeline with the peripherally restricted muscarinic receptor antagonist trospium chloride with the goal of ameliorating xanomeline-related adverse events associated with peripheral muscarinic receptors. The EMERGENT-2 trial aimed to assess the efficacy and safety of KarXT in people with schizophrenia experiencing acute psychosis.

Methods

EMERGENT-2 was a randomised, double-blind, placebo-controlled, flexible-dose, 5-week, inpatient, phase 3 trial in people with schizophrenia. Participants were adults aged 18–65 years with a diagnosis of schizophrenia who had a recent worsening of psychosis warranting hospital admission, a Positive and Negative Syndrome Scale (PANSS) score of 80 or higher, and a Clinical Global Impression-Severity score of 4 or higher. The participants were recruited from 22 inpatient sites in the USA, and were randomly assigned (1:1) to KarXT or placebo twice per day. Participants randomly assigned to KarXT received 50 mg xanomeline and 20 mg trospium twice per day for the first 2 days and then 100 mg xanomeline and 20 mg trospium twice per day for days 3–7. Beginning on day 8, KarXT dosing was flexible with an optional increase to 125 mg xanomeline and 30 mg trospium twice per day and the option to return to 100 mg xanomeline and 20 mg trospium based on tolerability. The primary endpoint was change from baseline to week 5 in PANSS total score. Efficacy analyses used the modified intention-to-treat population (all randomly assigned participants who received at least one trial medication dose and had at least one post-baseline PANSS assessment). Least squares mean change from baseline, SE, and least squares mean difference between the KarXT and placebo groups at week 5, along with the 95% CI and two-sided p values were calculated for the primary and secondary continuous efficacy endpoints. Safety analyses included all participants receiving at least one trial medication dose and used descriptive statistics. This trial is registered with ClinicalTrials.gov (NCT04659161).

Findings

From Dec 16, 2020, to April 13, 2022, of 407 people who were screened, 252 participants meeting enrolment criteria were randomly assigned to the KarXT (n=126) or placebo (n=126). Baseline PANSS total scores were 98·3 (KarXT; n=126) and 97·9 (placebo; n=125). The trial met the primary endpoint with a mean change from baseline to week 5 in PANSS total score that favoured KarXT (–21·2 points, SE 1·7) versus placebo (–11·6 points, 1·6; least squares mean difference –9·6; 95% CI –13·9 to –5·2; p<0·0001, Cohen's d effect size=0·61). All secondary endpoints were also met, and favoured KarXT versus placebo (p<0·05). The most common adverse events with KarXT versus placebo were constipation (27 [21%] vs 13 [10%]), dyspepsia (24 [19%] vs 10 [8%]), headache (17 [14%] vs 15 [12%]), nausea (24 [19%] vs seven [6%]), vomiting (18 [14%] vs one [1%]), hypertension (12 [10%] vs one [1%]), dizziness (11 [9%] vs four [3%]), gastro-oesophageal reflux disease (eight [6%] vs zero [0%]), and diarrhoea (seven [6%] vs four [3%]). Treatment-emergent adverse event rates of extrapyramidal motor symptoms (KarXT, zero [0%] vs placebo, zero [0%]), akathisia (one [1%] vs one [1%]), weight gain (zero [0%] vs one [1%]), and somnolence (six [5%] vs five [4%]) were similar between the KarXT and placebo groups, as were adverse event-related discontinuation rates (nine [7%] vs seven [6%]).

Interpretation

In the EMERGENT-2 trial, KarXT was effective in reducing positive and negative symptoms and was generally well tolerated. These results support the potential for KarXT to represent a new class of effective and well tolerated antipsychotic medicines based on activating muscarinic receptors, not the D2 dopamine receptor-blocking mechanism of all current antipsychotic medications. Results from additional trials, including the identical EMERGENT-3 trial and the 52-week, open-label EMERGENT-4 and EMERGENT-5 trials, will provide additional information on the efficacy and safety of KarXT in people with schizophrenia.

Funding

Karuna Therapeutics.

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