Efficacy of inflammation-based stratification for add-on celecoxib or minocycline in major depressive disorder: Protocol of the INSTA-MD double-blind placebo-controlled randomised clinical trial

IF 3.7 Q2 IMMUNOLOGY
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引用次数: 0

Abstract

Introduction

Different lines of evidence confirm the involvement of the immune system in the pathophysiology of major depressive disorder. Up to 30% of depressed patients present with an immune-mediated subtype, characterized by peripheral inflammation (high-sensitive C-reactive protein (hsCRP) ≥ 3 mg/l) and an atypical symptom profile with fatigue, anhedonia, increased appetite, and hypersomnia. This immune-mediated subtype of MDD is associated with poorer response to first-line antidepressant treatment. Consequently, strategies for immune-targeted augmentation should be prioritised towards patients with this subtype. Meta-analyses have shown modest but heterogeneous treatment effects with immune-targeted augmentation in unstratified MDD cohorts, with celecoxib and minocycline as most promising first-line treatment options. However, no study has prospectively evaluated the effectiveness of a priori stratification by baseline inflammation levels for add-on celecoxib or minocycline in MDD.

Methods

The INSTA-MD trial is a multicentre, 12-week, randomised, double-blind, placebo-controlled, parallel-group stratified clinical trial of adjunctive minocycline or celecoxib to treatment-as-usual for patients with MDD. Two hundred forty adult patients with Major Depressive Disorder who failed to remit with one or two trials of antidepressant treatment will be enrolled and allocated to high-hsCRP (hsCRP ≥3 mg/L) or low-hsCRP (hsCRP <3 mg/L) strata, where disproportional stratified sampling will ensure equally sized strata. Participants in each hsCRP stratum will be randomised to augment their ongoing antidepressant treatment with either adjunctive minocycline, celecoxib or placebo for a duration of 12 weeks, resulting in six treatment arms of each 40 participants. The primary objective is to evaluate the efficacy of immune-targeted augmentation with minocycline or celecoxib versus placebo, and the use of baseline hsCRP stratification to predict treatment response. Additionally, we will perform a head-to-head analysis between the two active compounds. The primary outcome measure is change in the Hamilton Depression Rating Scale (HDRS-17) total score. Secondary outcome measures will be response and remission rates, and change in inflammation-specific symptoms, adverse events and therapy acceptability (adherence). Further exploratory analyses will be performed with an array of peripheral inflammatory biomarkers, metabolic outcomes and physiological data.

Expected impact

The aim of INSTA-MD is to advance the use of immune-targeted precision psychiatry, by supporting the implementation of targeted hsCRP screening and treatment of immune-mediated MDD as a cost-effective intervention in primary care settings. Based on previous studies, we expect immune-targeted augmentation with minocycline or celecoxib to yield a superior remission rate of 15–30% compared to treatment as usual for immune-mediated cases of MDD. By treating immune-related depression early in the treatment algorithm with repurposed first-line anti-inflammatory treatments, we can significantly improve the outcomes of these patients, and reduce the global societal and economic burden of depression.

Ethics and dissemination

This protocol has been approved by the Medical Ethics Review Board (CTR - 04/08/2023)

Registration details

Trial registration number NCT05644301 (Clinical trial.gov), EU-CT 2022-501692-35-00.

基于炎症分层的塞来昔布或米诺环素对重度抑郁症的疗效:INSTA-MD双盲安慰剂对照随机临床试验方案
导言:不同的证据证实,免疫系统参与了重度抑郁症的病理生理学。多达 30% 的抑郁症患者表现为免疫介导亚型,其特征是外周炎症(高敏 C 反应蛋白 (hsCRP) ≥ 3 mg/l)和非典型症状,包括疲劳、厌食、食欲增加和嗜睡。这种由免疫介导的亚型 MDD 对一线抗抑郁治疗的反应较差。因此,针对这一亚型患者的免疫增强策略应优先考虑。Meta 分析表明,在未分层的 MDD 队列中,免疫靶向增效疗法的治疗效果一般,但也不尽相同,其中塞来昔布和米诺环素是最有前景的一线治疗方案。方法INSTA-MD试验是一项多中心、为期12周、随机、双盲、安慰剂对照、平行组分层临床试验,对MDD患者在常规治疗的基础上辅助米诺环素或塞来昔布进行治疗。我们将招募 240 名经一或两次抗抑郁治疗试验均未缓解的成年重度抑郁症患者,并将其分配到高 hsCRP(hsCRP ≥3 mg/L)或低 hsCRP(hsCRP <3 mg/L)分层中,其中比例失调分层抽样将确保分层规模相等。每个 hsCRP 分层中的参与者将随机接受米诺环素、塞来昔布或安慰剂的辅助治疗,为期 12 周。主要目的是评估米诺环素或塞来昔布与安慰剂的免疫靶向增强疗效,以及使用基线 hsCRP 分层预测治疗反应。此外,我们还将对两种活性化合物进行对比分析。主要结果指标是汉密尔顿抑郁量表(HDRS-17)总分的变化。次要结果指标将包括应答率和缓解率,以及炎症特异性症状、不良反应和治疗可接受性(依从性)的变化。INSTA-MD的目标是通过支持实施有针对性的hsCRP筛查和治疗免疫介导的MDD,将其作为初级医疗机构中一项具有成本效益的干预措施,从而推动免疫靶向精准精神病学的应用。根据以往的研究,我们预计与常规治疗相比,使用米诺环素或塞来昔布进行免疫靶向增效治疗可使免疫介导的 MDD 病例的缓解率提高 15-30%。通过在治疗算法的早期使用重新设计的一线抗炎疗法治疗免疫相关抑郁症,我们可以显著改善这些患者的预后,并减轻抑郁症对全球社会和经济造成的负担。伦理与传播本方案已获得医学伦理审查委员会批准(CTR - 04/08/2023)注册详细信息试验注册号NCT05644301(Clinical trial.gov),EU-CT 2022-501692-35-00。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Brain, behavior, & immunity - health
Brain, behavior, & immunity - health Biological Psychiatry, Behavioral Neuroscience
CiteScore
8.50
自引率
0.00%
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审稿时长
97 days
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