首页> 美国卫生研究院文献>Journal of Virology >Screening Random Peptide Libraries with Subacute Sclerosing Panencephalitis Brain-Derived Recombinant Antibodies Identifies Multiple Epitopes in the C-Terminal Region of the Measles Virus Nucleocapsid Protein
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Screening Random Peptide Libraries with Subacute Sclerosing Panencephalitis Brain-Derived Recombinant Antibodies Identifies Multiple Epitopes in the C-Terminal Region of the Measles Virus Nucleocapsid Protein

机译:亚急性硬化性全脑炎脑源性重组抗体筛选随机肽文库可识别麻疹病毒核蛋白C末端区域的多个表位

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摘要

Infectious and inflammatory diseases of the CNS are often characterized by a robust B-cell response that manifests as increased intrathecal immunoglobulin G (IgG) synthesis and the presence of oligoclonal bands. We previously used laser capture microdissection and single-cell PCR to analyze the IgG variable regions of plasma cells from the brain of a patient with subacute sclerosing panencephalitis (SSPE). Five of eight human IgG1 recombinant antibodies (rAbs) derived from SSPE brain plasma cell clones recognized the measles virus (MV) nucleocapsid protein, confirming that the antibody response in SSPE targets primarily the agent causing disease. In this study, as part of our work on antigen identification, we used four rAbs to probe a random phage-displayed peptide library to determine if epitopes within the MV nucleocapsid protein could be identified with SSPE brain rAbs. All four of the SSPE rAbs enriched phage-displayed peptide sequences that reacted specifically to their panning rAb by enzyme-linked immunosorbent assay. BLASTP searches of the NCBI protein database revealed clear homologies in three peptides and different amino acid stretches within the 65 C-terminal amino acids of the MV nucleocapsid protein. The specificities of SSPE rAbs to these regions of the MV nucleocapsid protein were confirmed by binding to synthetic peptides or to short cDNA expression products. These results indicate the feasibility of using peptide screening for antigen discovery in central nervous system inflammatory diseases of unknown etiology, such as multiple sclerosis, neurosarcoidosis, or Behcet's syndrome.
机译:中枢神经系统的感染性和炎性疾病通常以强大的B细胞反应为特征,表现为鞘内免疫球蛋白G(IgG)合成增加和寡克隆带的存在。我们以前使用激光捕获显微切割和单细胞PCR分析亚急性硬化性全脑炎(SSPE)患者大脑中浆细胞的IgG可变区。源自SSPE脑浆细胞克隆的八种人IgG1重组抗体(rAb)中的五种识别了麻疹病毒(MV)核衣壳蛋白,从而证实SSPE中的抗体反应主要针对引起疾病的物质。在这项研究中,作为我们抗原鉴定工作的一部分,我们使用了四个rAb来探测随机噬菌体展示的肽库,以确定用SSPE脑rAb是否可以鉴定MV核衣壳蛋白内的表位。所有四个SSPE rAb均富集了噬菌体展示的肽序列,这些序列通过酶联免疫吸附测定对其淘选rAb特异性反应。 BLASTP搜索NCBI蛋白质数据库揭示了MV核衣壳蛋白65个C末端氨基酸中三个肽段和不同氨基酸段的清晰同源性。通过与合成肽或短cDNA表达产物结合,可以确定SSPE rAb对MV核衣壳蛋白这些区域的特异性。这些结果表明在病因不明的中枢神经系统炎性疾病(例如多发性硬化症,神经结节病或白塞氏综合症)中使用肽筛查进行抗原发现的可行性。

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