Audran Régine, Karoui Olfa, Donnet Laura, Soumas Vassili, Fares Fady, Lovis Alban, Noirez Leslie, Cavassini Matthias, Fayet-Mello Aurélie, Satti Iman, McShane Helen, Spertini François
Department of Medicine, Division of Allergy and Immunology, Centre Hospitalier Universitaire Vaudois (CHUV), Lausanne, Switzerland.
Clinical Trial Unit, Centre Hospitalier Universitaire Vaudois (CHUV) and University of Lausanne, Lausanne, Switzerland.
J Infect. 2024 Aug;89(2):106205. doi: 10.1016/j.jinf.2024.106205. Epub 2024 Jun 17.
A BCG booster vaccination administered via the respiratory mucosa may establish protective immune responses at the primary site of Mycobacterium tuberculosis infection. The primary objective of this trial was to compare the safety and immunogenicity of inhaled versus intramuscular administered ChAdOx1-85A.
We conducted a single-centre, randomised, double-blind, controlled phase 1 study (Swiss National Clinical Trials Portal number SNCTP000002920). After a dose-escalation vaccination in nine BCG-vaccinated healthy adults, a dose of 1 × 10 vp of ChAdOx1-85A was administered to twenty BCG-vaccinated adults that were randomly allocated (1:1) into two groups: aerosol ChAdOx1-85A with intramuscular saline placebo or intramuscular ChAdOx1-85A with aerosol saline placebo, using block randomisation. A control group of ten BCG-naïve adults received aerosol ChAdOx1-85A at the same dose. Primary outcomes were solicited and unsolicited adverse events (AEs) up to day 16 post-vaccination and Serious AEs (SAEs) up to 24 weeks; secondary outcomes were cell-mediated and humoral immune responses in blood and bronchoalveolar lavage (BAL) samples.
Both vaccination routes were well tolerated with no SAEs. Intramuscular ChAdOx1-85A was associated with more local AEs (mostly pain at the injection site) than aerosol ChAdOx1-85A. Systemic AEs occurred in all groups, mainly fatigue and headaches, without differences between groups. Respiratory AEs were not different between BCG-vaccinated groups. Aerosol ChAdOx1-85A vaccination induced Ag85A BAL and systemic cellular immune responses with compartmentalisation of the immune responses: aerosol ChAdOx1-85A induced stronger BAL cellular responses, particularly IFNγ/IL17+CD4+ T cells; intramuscular ChAdOx1-85A induced stronger systemic cellular and humoral responses.
Inhaled ChAdOx1-85A was well-tolerated and induced lung mucosal and systemic Ag85A-specific T-cell responses. These data support further evaluation of aerosol ChAdOx1-85A and other viral vectors as a BCG-booster vaccination strategy.
通过呼吸道黏膜接种卡介苗加强针可能在结核分枝杆菌感染的主要部位建立保护性免疫反应。本试验的主要目的是比较吸入式与肌肉注射式ChAdOx1-85A的安全性和免疫原性。
我们开展了一项单中心、随机、双盲、对照的1期研究(瑞士国家临床试验门户网站编号SNCTP000002920)。在9名接种卡介苗的健康成年人中进行剂量递增接种后,将1×10 vp的ChAdOx1-85A给予20名接种卡介苗的成年人,这些成年人被随机分配(1:1)为两组:雾化吸入ChAdOx1-85A并肌肉注射生理盐水安慰剂,或肌肉注射ChAdOx1-85A并雾化吸入生理盐水安慰剂,采用区组随机化。10名未接种卡介苗的成年人组成的对照组接受相同剂量的雾化吸入ChAdOx1-85A。主要结局为接种疫苗后第16天的主动和被动不良事件(AE)以及24周内的严重不良事件(SAE);次要结局为血液和支气管肺泡灌洗(BAL)样本中的细胞介导免疫和体液免疫反应。
两种接种途径耐受性良好,均未出现严重不良事件。与雾化吸入ChAdOx1-85A相比,肌肉注射ChAdOx1-85A出现的局部不良事件更多(主要是注射部位疼痛)。所有组均出现全身性不良事件,主要为疲劳和头痛,组间无差异。接种卡介苗的组之间呼吸道不良事件无差异。雾化吸入ChAdOx1-85A疫苗接种诱导了Ag85A BAL和全身性细胞免疫反应,且免疫反应存在分区:雾化吸入ChAdOx1-85A诱导更强的BAL细胞反应,尤其是IFNγ/IL17+CD4+ T细胞;肌肉注射ChAdOx1-85A诱导更强的全身性细胞和体液反应。
雾化吸入ChAdOx1-85A耐受性良好,并诱导了肺部黏膜和全身性Ag85A特异性T细胞反应。这些数据支持进一步评估雾化吸入ChAdOx1-85A和其他病毒载体作为卡介苗加强针接种策略。
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