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微阵列肽免疫分析的 IgE 和 IgG 表位作图揭示了 IgG3 马免疫球蛋白的免疫反应的重要性和多样性。

IgE and IgG epitope mapping by microarray peptide-immunoassay reveals the importance and diversity of the immune response to the IgG3 equine immunoglobulin.

机构信息

Center for Technological Development in Health (CDTS) National Institute of Science and Technology for Innovation in Neglected Diseases (INCT-IDN), FIOCRUZ, Rio de Janeiro, RJ, Brazil; Molecular and Cellular Biology Department, Federal Fluminense University, Niterói, RJ, Brazil.

Molecular and Cellular Biology Department, Federal Fluminense University, Niterói, RJ, Brazil.

出版信息

Toxicon. 2014 Feb;78:83-93. doi: 10.1016/j.toxicon.2013.12.001. Epub 2013 Dec 13.

DOI:10.1016/j.toxicon.2013.12.001
PMID:24334152
Abstract

The presence of whole horse IgG in therapeutic snake antivenom preparations of high purity is a contamination that can cause IgE-mediated allergic reactions in patients. In this study, the immunodominant IgE and IgG-binding epitopes in horse heavy chain IgG3 were mapped using arrays of overlapping peptides synthesized directly onto activated cellulose membranes. Pooled human sera from patients with and without horse antivenom allergies were used to probe the membrane. We have demonstrated that, for both cases, individuals produce antibodies to epitopes of sequential amino acids of horse heavy chain IgG3, although the signal strength and specificity appear to be distinct between the two groups of patients. A single region was found to contain the dominant allergic IgE epitope. The critical residues involved in the binding of human IgE to the epitope were determined to include four hydrophobic amino acids followed by polar and charged residues that formed a coil structure. This is the first study to describe the specific amino acid sequences involved with the immune recognition of human IgG and IgE to horse antivenom.

摘要

高纯度治疗性蛇抗蛇毒血清制剂中存在完整马 IgG 是一种污染,可导致患者发生 IgE 介导的过敏反应。在这项研究中,使用直接合成在活化纤维素膜上的重叠肽阵列来绘制马重链 IgG3 的免疫优势 IgE 和 IgG 结合表位。使用来自有和没有马抗蛇毒血清过敏的患者的混合血清来探测膜。我们已经证明,对于这两种情况,个体都产生针对马重链 IgG3 的连续氨基酸表位的抗体,尽管两组患者的信号强度和特异性似乎不同。发现一个单一区域包含主要的过敏 IgE 表位。确定了与人类 IgE 结合到该表位相关的关键残基包括四个疏水性氨基酸,其后是形成螺旋结构的极性和带电残基。这是首次描述与人 IgG 和 IgE 对马抗蛇毒血清的免疫识别相关的特定氨基酸序列的研究。

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