mRNA Galsomes Vaccine Protects Budgerigars Against Virulent Chlamydia psittaci Challenge.

IF 5.2 3区 医学 Q1 IMMUNOLOGY Vaccines Pub Date : 2025-02-19 DOI:10.3390/vaccines13020206
Anne De Meyst, Joeri Van Mieghem, Koen Chiers, Koen Raemdonck, Rein Verbeke, Ine Lentacker, Daisy Vanrompay
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Abstract

Background/objectives: Chlamydia (C.) psittaci is an avian respiratory pathogen that regularly infects budgerigars (Melopsittacus undulatus) and is a known zoonosis. This study aimed to evaluate the efficacy of a nucleoside-modified mRNA vaccine formulated in lipid nanoparticles (LNPs), either with (mRNA Galsomes) or without (mRNA LNPs) the glycolipid antigen α-Galactosylceramide, in protecting budgerigars against C. psittaci genotype A infection.

Methods: Three groups of eight budgerigars received two intramuscular vaccinations with PBS, mRNA LNPs or mRNA Galsomes, and were subsequently challenged via aerosol with the C. psittaci genotype A strain 90/1051. Vaccine efficacy was assessed over 14 days post challenge by monitoring clinical signs, macroscopic and microscopic lesions, pathogen excretion and chlamydial burden in organs. Antibody levels were evaluated at baseline, after vaccination and post challenge.

Results: Both mRNA LNPs and mRNA Galsomes induced significant serum antibody responses post booster. Vaccination significantly reduced clinical signs, chlamydial burden in the lungs and macroscopic lesions in conjunctiva, conchae, lungs and thoracic airsacs, compared to controls. Additionally, mRNA Galsomes-treated birds showed a significantly reduced lung inflammation and fewer macroscopic lesions in abdominal airsacs and liver, compared to non-vaccinated animals. These animals also experienced a significantly lower chlamydial burden in the spleen, fewer clinical signs at day 11 and fewer fecal shedding at day 14 post challenge, compared to mRNA LNP-treated animals.

Conclusions: This study demonstrated that mRNA vaccination confers partial protection against C. psittaci in budgerigars, with mRNA Galsomes appearing to provide enhanced efficacy. However, the absence of species-specific reagents for assessing cellular immunity in Psittaciformes limits a comprehensive understanding of vaccine-induced protection. The development of psittacine-specific T cell markers and cytokine assays is necessary to further elucidate immune mechanisms and optimize vaccine formulations.

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mRNA Galsomes疫苗保护虎皮鹦鹉免受鹦鹉热衣原体的攻击。
背景/目的:鹦鹉热衣原体(C.)是一种禽呼吸道病原体,通常感染虎皮猴(波状斑鹦鹉),是一种已知的人畜共患病。本研究旨在评估核苷修饰的mRNA疫苗在脂质纳米颗粒(LNPs)中制备的效果,无论是含有(mRNA Galsomes)还是不含(mRNA LNPs)糖脂抗原α-半乳糖神经酰胺,以保护鹦鹉鹦鹉免受基因型a感染。方法:3组8只虎皮鹦鹉分别用PBS、mRNA LNPs和mRNA Galsomes分别肌肉接种2次,然后用90/1051鹦鹉螺基因型A菌株气溶胶攻毒。接种后14天,通过监测临床症状、肉眼和显微镜下病变、病原体排泄和器官内衣原体负荷来评估疫苗效果。在基线、接种疫苗后和攻毒后评估抗体水平。结果:mRNA LNPs和mRNA Galsomes增强后均诱导显著的血清抗体应答。与对照组相比,疫苗接种显著减少了临床症状、肺部衣原体负担和结膜、耳蜗、肺和胸廓气囊的宏观病变。此外,与未接种疫苗的动物相比,mRNA galsome治疗的鸟类表现出明显减少的肺部炎症和腹部气囊和肝脏的宏观病变。与mRNA lnp处理的动物相比,这些动物的脾脏衣原体负荷也显著降低,第11天的临床症状更少,第14天的粪便脱落也更少。结论:本研究表明,mRNA疫苗接种对虎皮鹦鹉具有部分保护作用,mRNA Galsomes似乎提供了增强的功效。然而,缺乏物种特异性试剂来评估鹦鹉形虫的细胞免疫,限制了对疫苗诱导的保护的全面了解。发展鹦鹉螺特异性T细胞标记物和细胞因子检测对于进一步阐明免疫机制和优化疫苗配方是必要的。
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来源期刊
Vaccines
Vaccines Pharmacology, Toxicology and Pharmaceutics-Pharmacology
CiteScore
8.90
自引率
16.70%
发文量
1853
审稿时长
18.06 days
期刊介绍: Vaccines (ISSN 2076-393X) is an international, peer-reviewed open access journal focused on laboratory and clinical vaccine research, utilization and immunization. Vaccines publishes high quality reviews, regular research papers, communications and case reports.
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