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新证实的主要过敏原Hum j 1的临床相关性及低致敏性肽的特性分析

Characterization of the clinical relevance and hypoallergenic peptides of the newly evidenced major allergen Hum j 1.

作者信息

Cheng Ya-Li, Li Qiong, Yang Yong-Shi, Hou Yi-Bo, Xu Zhi-Qiang, Wei Ji-Fu, Sun Jin-Lyu

机构信息

Department of Allergy, State Key Laboratory of Complex Severe and Rare Diseases, Peking Union Medical College Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing, China.

Department of Pharmacy, The Affiliated Cancer Hospital of Nanjing Medical University and Jiangsu Cancer Hospital and Jiangsu Institute of Cancer Research, Nanjing, China.

出版信息

Front Immunol. 2025 Jun 23;16:1588870. doi: 10.3389/fimmu.2025.1588870. eCollection 2025.

Abstract

BACKGROUND

(HJ) pollen is a predominant autumn allergen in northern China. Two decades ago, a 10 kDa protein termed Hum j 1 was proposed as a major allergen, but its uncertainty hindered its clinical application. This study aims to investigate the clinical relevance of Hum j 1 and screen hypoallergenic peptides for potential application in molecular diagnosis and immunotherapy.

METHODS

Serum samples from 93 HJ pollen-allergic patients were analyzed for IgE reactivity against recombinant Hum j 1 (rHum j 1). We evaluated correlations between IgE responses to rHum j 1 and HJ pollen crude extracts using Spearman's rank correlation analysis. The association between clinical symptoms and Hum j 1-IgE positivity was evaluated by group comparisons and multivariable analyses. Allergenicity of Hum j 1 was further investigated by immunoblotting and basophil activation tests. Six KLH-coupled peptides (21-25 amino acids) spanning the complete Hum j 1 sequence were synthesized to assess hypoallergenicity and IgG-mediated inhibitory effects against allergen-specific IgE binding using a murine passive immunization model.

RESULTS

rHum j 1 demonstrated IgE reactivity in 74.2% (69/93) of the patients and induced significant basophil activation. rHum j 1-specific IgE levels showed a moderate positive correlation with crude extract-specific IgE levels (Spearman's ρ = 0.529, < 0.0001). Patients with allergic rhinitis complicated by asthma had significantly higher levels of Hum j 1-sIgE ( = 0.014). We found a significant association between Hum j 1 sensitization and asthma in the multivariate analysis [odds ratio (OR) = 3.98, 95% confidence interval (CI): 1.2-13.0, = 0.02], with Hum j 1-sensitized patients showing higher asthma prevalence compared to non-sensitized individuals (46% vs. 17%, = 0.010). All six peptides showed significantly reduced IgE reactivity ( < 0.0001) and minimal basophil activation. Immunized mice produced high-titer IgG antibodies that inhibited patient IgE binding to rHum j 1 by 22.09%-64.61%.

CONCLUSIONS

Hum j 1 could enhance the sensitivity of HJ pollen crude extract-based IgE assays. IgE reactivity to Hum j 1 was more frequently associated with allergic asthma. The hypoallergenic linear peptides of Hum j 1 laid the foundation for the development of a molecular vaccine for allergen-specific immunotherapy. These findings would contribute to developing diagnostic and therapeutic strategies for HJ pollinosis.

摘要

背景

(HJ)花粉是中国北方秋季主要的过敏原。二十年前,一种名为Hum j 1的10 kDa蛋白被提出作为主要过敏原,但其不确定性阻碍了其临床应用。本研究旨在探讨Hum j 1的临床相关性,并筛选低变应原性肽,以用于分子诊断和免疫治疗的潜在应用。

方法

分析93例HJ花粉过敏患者的血清样本对重组Hum j 1(rHum j 1)的IgE反应性。我们使用Spearman等级相关分析评估了对rHum j 1的IgE反应与HJ花粉粗提物之间的相关性。通过组间比较和多变量分析评估临床症状与Hum j 1-IgE阳性之间的关联。通过免疫印迹和嗜碱性粒细胞活化试验进一步研究Hum j 1的变应原性。合成了六种跨越完整Hum j 1序列的KLH偶联肽(21 - 25个氨基酸),以使用小鼠被动免疫模型评估低变应原性和IgG介导的对过敏原特异性IgE结合的抑制作用。

结果

rHum j 1在74.2%(69/93)的患者中表现出IgE反应性,并诱导显著的嗜碱性粒细胞活化。rHum j 1特异性IgE水平与粗提物特异性IgE水平呈中度正相关(Spearman's ρ = 0.529,< 0.0001)。过敏性鼻炎合并哮喘的患者Hum j 1-sIgE水平显著更高(= 0.014)。在多变量分析中,我们发现Hum j 1致敏与哮喘之间存在显著关联[比值比(OR)= 3.98,95%置信区间(CI):1.2 - 13.0,= 0.02],与未致敏个体相比,Hum j 1致敏患者的哮喘患病率更高(46%对17%,= 0.010)。所有六种肽均表现出显著降低的IgE反应性(< 0.0001)和最小的嗜碱性粒细胞活化。免疫小鼠产生了高滴度的IgG抗体,可抑制患者IgE与rHum j 1的结合达22.09% - 64.61%。

结论

Hum j 1可提高基于HJ花粉粗提物的IgE检测的敏感性。对Hum j 1的IgE反应性更常与过敏性哮喘相关。Hum j 1的低变应原性线性肽为开发用于过敏原特异性免疫治疗的分子疫苗奠定了基础。这些发现将有助于制定HJ花粉症的诊断和治疗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ee75/12230049/514f3cfda6f2/fimmu-16-1588870-g001.jpg

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