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美洲大蠊Per a 9过敏原的分子克隆、表达、IgE结合活性及计算机模拟表位预测

Molecular cloning, expression, IgE binding activities and in silico epitope prediction of Per a 9 allergens of the American cockroach.

作者信息

Yang Haiwei, Chen Hao, Jin Min, Xie Hua, He Shaoheng, Wei Ji-Fu

机构信息

Allergy and Clinical Immunology Research Centre, The First Affiliated Hospital of Liaoning Medical University, Jinzhou, Liaoning 121001, P.R. China.

Research Division of Clinical Pharmacology, The First Affiliated Hospital of Nanjing Medical University, Nanjing, Jiangsu 210029, P.R. China.

出版信息

Int J Mol Med. 2016 Dec;38(6):1795-1805. doi: 10.3892/ijmm.2016.2793. Epub 2016 Oct 27.

Abstract

Per a 9 is a major allergen of the American cockroach (CR), which has been recognized as an important cause of imunoglobulin E-mediated type I hypersensitivity worldwide. However, it is not neasy to obtain a substantial quantity of this allergen for use in functional studies. In the present study, the Per a 9 gene was cloned and expressed in Escherichia coli (E. coli) systems. It was found that 13/16 (81.3%) of the sera from patients with allergies caused by the American CR reacted to Per a 9, as assessed by enzyme-linked immunosorbent assay, confirming that Per a 9 is a major allergen of CR. The induction of the expression of CD63 and CCR3 in passively sensitized basophils (from sera of patients with allergies caused by the American CR) by approximately 4.2-fold indicated that recombinant Per a 9 was functionally active. Three immunoinformatics tools, including the DNAStar Protean system, Bioinformatics Predicted Antigenic Peptides (BPAP) system and the BepiPred 1.0 server were used to predict the potential B cell epitopes, while Net-MHCIIpan-2.0 and NetMHCII-2.2 were used to predict the T cell epitopes of Per a 9. As a result, we predicted 11 peptides (23-28, 39-46, 58-64, 91-118, 131-136, 145-154, 159-165, 176-183, 290-299, 309-320 and 338-344) as potential B cell linear epitopes. In T cell prediction, the Per a 9 allergen was predicted to have 5 potential T cell epitope sequences, 119-127, 194-202, 210-218, 239-250 and 279-290. The findings of our study may prove to be useful in the development of peptide-based vaccines to combat CR-induced allergies.

摘要

变应原Per a 9是美洲大蠊的一种主要变应原,在全球范围内,它已被公认为是免疫球蛋白E介导的I型超敏反应的一个重要病因。然而,要获得大量这种变应原用于功能研究并非易事。在本研究中,Per a 9基因在大肠杆菌系统中被克隆并表达。通过酶联免疫吸附测定评估发现,16份因美洲大蠊引起过敏的患者血清中有13份(81.3%)与Per a 9发生反应,证实Per a 9是美洲大蠊的一种主要变应原。重组Per a 9使被动致敏嗜碱性粒细胞(来自因美洲大蠊引起过敏的患者血清)中CD63和CCR3的表达诱导增加约4.2倍,表明重组Per a 9具有功能活性。使用三种免疫信息学工具,包括DNAStar Protean系统、生物信息学预测抗原肽(BPAP)系统和BepiPred 1.0服务器来预测潜在的B细胞表位,同时使用Net-MHCIIpan-2.0和NetMHCII-2.2来预测Per a 9的T细胞表位。结果,我们预测了11个肽段(23 - 28、39 - 46、58 - 64、91 - 118、131 - 136、145 - 154、159 - 165、176 - 183、290 - 299、309 - 320和338 - 344)作为潜在的B细胞线性表位。在T细胞预测中,预测Per a 9变应原有5个潜在的T细胞表位序列,即119 - 127、194 - 202、210 - 218、239 - 250和279 - 290。我们的研究结果可能在开发基于肽段的疫苗以对抗美洲大蠊引起的过敏方面证明是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d381/5117749/4e0aaa42926f/IJMM-38-06-1795-g00.jpg

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