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鉴定 Bermuda 草花粉主要过敏原 Cyn d 1 的 IgE 和 IgG4 抗体结合表位

Mapping of IgE and IgG4 antibody-binding epitopes in Cyn d 1, the major allergen of Bermuda grass pollen.

机构信息

Children's Medical Center, Taipei Veterans General Hospital, Taipei, Taiwan.

出版信息

Int Arch Allergy Immunol. 2012;157(2):125-35. doi: 10.1159/000327544. Epub 2011 Oct 5.

DOI:10.1159/000327544
PMID:21985791
Abstract

BACKGROUND

Bermuda grass pollen (BGP) is an important seasonal aeroallergen worldwide which induces allergic disorders such as allergic rhinitis, conjunctivitis and asthma. Cyn d 1 is the major allergen of BGP. This study is aimed to map human IgE and IgG(4) antibody-binding sequential epitopes on Cyn d 1 by dot immunoblotting.

METHODS

Synthetic peptides (10-mers; 5 overlapping residues) spanning the full length of Cyn d 1 were used for dot immunoblotting to map human IgE and IgG(1-4) antibody-binding regions with sera from BGP-allergic patients. Synthetic peptides with more overlapping residues were used for further mapping. Essential amino acids in each epitope were examined by single amino acid substitution with alanine. Peptides with sequence polymorphism of epitopes of Cyn d 1 were also synthesized to extrapolate their differences in binding capability.

RESULTS

Four major IgE-binding epitopes (peptides 15(-1), 21, 33(-2) and 35(+1), corresponding to amino acids 70-79, 101-110, 159-167 and 172-181) and 5 major IgG(4)-binding epitopes (peptides 15(-1), 30(-2), 33(-2), 35(+1) and 39, corresponding to amino acids 70-79, 144-153, 159-167, 172-181 and 192-200) were identified. They are all located on the surface of the simulated Cyn d 1 molecule, and three of them are major epitopes for both IgE and IgG(4). Their critical amino acids were all characterized. Major epitopes for human IgG(1) to IgG(4) are almost identical.

CONCLUSIONS

This is the first study to map the sequential epitopes for human IgE and IgG(4) subclasses in Cyn d 1. It will be helpful for future development in immunotherapy and diagnosis.

摘要

背景

百慕大草花粉(BGP)是全球重要的季节性气传过敏原,可引起过敏性疾病,如过敏性鼻炎、结膜炎和哮喘。Cyn d 1 是 BGP 的主要过敏原。本研究旨在通过斑点免疫印迹法绘制 Cyn d 1 上人类 IgE 和 IgG(4)抗体结合的顺序表位。

方法

使用全长 Cyn d 1 的合成肽(10 个氨基酸;5 个重叠残基)进行斑点免疫印迹,以绘制 BGP 过敏患者血清中与人类 IgE 和 IgG(1-4)抗体结合的区域。使用具有更多重叠残基的合成肽进行进一步作图。通过用丙氨酸取代每个表位的必需氨基酸来检查。还合成了具有 Cyn d 1 表位序列多态性的肽,以推断其结合能力的差异。

结果

鉴定出 4 个主要的 IgE 结合表位(肽 15(-1)、21、33(-2)和 35(+1),对应于氨基酸 70-79、101-110、159-167 和 172-181)和 5 个主要的 IgG(4)结合表位(肽 15(-1)、30(-2)、33(-2)、35(+1)和 39,对应于氨基酸 70-79、144-153、159-167、172-181 和 192-200)。它们都位于模拟 Cyn d 1 分子的表面,其中 3 个是 IgE 和 IgG(4)的主要表位。它们的关键氨基酸都有特征。人类 IgG(1)至 IgG(4)的主要表位几乎相同。

结论

这是首次绘制 Cyn d 1 上人类 IgE 和 IgG(4)亚类的顺序表位的研究。它将有助于未来的免疫治疗和诊断发展。

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