Institute of Immunology, Faculty of Veterinary Medicine, Leipzig University, Leipzig, Germany.
Institute of Bacteriology and Mycology, Faculty of Veterinary Medicine, Leipzig University, Leipzig, Germany.
Front Immunol. 2024 Feb 29;15:1347164. doi: 10.3389/fimmu.2024.1347164. eCollection 2024.
Severe equine asthma (SEA) is a common chronic disease of adult horses with characteristic recurrent airway obstruction and similarities to neutrophilic asthma in humans. As an extrinsic stimulus, hay dust exposure is a major risk factor and induces acute exacerbation in susceptible horses. However, single inducing agents of SEA have hardly been identified on a molecular basis. () is a common mold species in hay and has been described as a major provoking agent of SEA.
Aiming to identify disease-relevant antigens, we analyzed using an immunoproteomics approach on two-dimensional immunoblots of protein probed with serum from environmentally matched asthmatic and healthy horses (n=5 pairs). binding serum immunoglobulins (Pan-Ig), and the isotypes IgG4/7 and IgG3/5 were quantified for each protein spot and then compared between asthmatic and healthy horses.
For 21 out of 289 spots serum immunoglobulin (Ig) binding was different between the two groups for Pan-Ig or the isotypes. If differences were detected, Pan-Ig and IgG4/7 binding to the proteins were lower, while IgG3/5 binding was higher in asthmatic than healthy horse sera. Proteins were extracted from the 21 spots of interest and analyzed by liquid chromatography mass spectrometry. Eight prioritized proteins (candidate antigens) were expressed as recombinant proteins. Some of these have been previously described as major or minor allergens, alongside other proteins, most with hydrolase activity. Recombinant candidate antigens were tested on 1D immunoblots to confirm their relevance as antigens by serum antibody binding. Four proteins (beta-hexosaminidase, class II aldolase/adducin domain protein, glucoamylase, peptide hydrolase B0XX53) showed different antibody binding characteristics between asthmatic and healthy horses and are likely relevant antigens in SEA. Their identification can provide the basis for innovative diagnostics, prevention, or therapeutic approaches. Additionally, a more profound understanding of SEA and its potential underlying mechanisms can be established. Elevated serum IgG3/5 antibodies correlate with T helper cell 2 responses in other equine pathologies, and the recombinant SEA antigens developed here can become instrumental in analyzing the involvement of SEA-specific T cell responses and Ig responses in future studies.
严重马气喘(SEA)是一种常见的成年马慢性疾病,具有特征性的复发性气道阻塞,与人的中性粒细胞性哮喘相似。作为一种外在刺激,干草粉尘暴露是一个主要的危险因素,并可诱发易感马的急性加重。然而,SEA 的单一诱导剂在分子基础上几乎没有被确定。()是干草中的一种常见霉菌,已被描述为 SEA 的主要诱发因素。
为了鉴定与疾病相关的抗原,我们使用免疫蛋白质组学方法在二维免疫印迹上分析了用来自环境匹配的哮喘和健康马的血清(n=5 对)探测的蛋白质。分析了与每种蛋白质斑点结合的 Pan-Ig 以及同种型 IgG4/7 和 IgG3/5,并将其在哮喘和健康马之间进行比较。
对于 289 个斑点中的 21 个,两组之间的 Pan-Ig 或同种型的血清免疫球蛋白(Ig)结合不同。如果检测到差异,则哮喘马血清中 Pan-Ig 和 IgG4/7 与蛋白质的结合降低,而 IgG3/5 的结合增加。从 21 个感兴趣的斑点中提取蛋白质,并通过液相色谱-质谱分析。优先选择 8 种蛋白质(候选抗原)作为重组蛋白表达。其中一些先前被描述为主要或次要过敏原,以及其他具有水解酶活性的蛋白质。在 1D 免疫印迹上测试重组候选抗原,以通过血清抗体结合来确认它们作为抗原的相关性。四种蛋白质(β-己糖胺酶、II 类醛缩酶/附加蛋白域蛋白、糖化酶、肽水解酶 B0XX53)显示哮喘和健康马之间不同的抗体结合特征,并且可能是 SEA 的相关抗原。它们的鉴定可以为创新的诊断、预防或治疗方法提供基础。此外,可以建立对 SEA 及其潜在潜在机制的更深入了解。在其他马的病理学中,升高的血清 IgG3/5 抗体与辅助性 T 细胞 2 反应相关,这里开发的重组 SEA 抗原可以成为分析 SEA 特异性 T 细胞反应和 Ig 反应在未来研究中的重要工具。
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