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首页> 外文期刊>The Journal of Infectious Diseases >Probing of a Human Proteome Microarray With a Recombinant Pathogen Protein Reveals a Novel Mechanism by Which Hookworms Suppress B-Cell Receptor Signaling
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Probing of a Human Proteome Microarray With a Recombinant Pathogen Protein Reveals a Novel Mechanism by Which Hookworms Suppress B-Cell Receptor Signaling

机译:人类蛋白质组微阵列与重组病原蛋白的探测揭示了钩虫抑制B细胞受体信号转导的新机制。

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Na-ASP-2 is an efficacious hookworm vaccine antigen. However, despite elucidation of its crystal structure and studies addressing its immunobiology, the function of Na-ASP-2 has remained elusive. We probed a 9000-protein human proteome microarray with Na-ASP-2 and showed binding to CD79A, a component of the B-cell antigen receptor complex. Na-ASP-2 bound to human B lymphocytes ex vivo and downregulated the transcription of approximately 1000 B-cell messenger RNAs (mRNAs), while only approximately 100 mRNAs were upregulated, compared with control-treated cells. The expression of a range of molecules was affected by Na-ASP-2, including factors involved in leukocyte transendothelial migration pathways and the B-cell signaling receptor pathway. Of note was the downregulated transcription of lyn and pi3k, molecules that are known to interact with CD79A and control B-cell receptor signaling processes. Together, these results highlight a previously unknown interaction between a hookworm-secreted protein and B cells, which has implications for helminth-driven immunomodulation and vaccine development. Further, the novel use of human protein microarrays to identify host-pathogen interactions, coupled with ex vivo binding studies and subsequent analyses of global gene expression in human host cells, demonstrates a new pipeline by which to explore the molecular basis of infectious diseases.
机译:Na-ASP-2是一种有效的钩虫疫苗抗原。然而,尽管阐明了其晶体结构和针对其免疫生物学的研究,但Na-ASP-2的功能仍然难以捉摸。我们用Na-ASP-2探测了9000种蛋白质的人蛋白质组微阵列,并显示出与CD79A的结合,CD79A是B细胞抗原受体复合物的组成部分。与对照处理的细胞相比,Na-ASP-2离体结合人B淋巴细胞并下调了约1000个B细胞信使RNA(mRNA)的转录,而仅上调了约100个mRNA。 Na-ASP-2影响了一系列分子的表达,其中包括与白细胞跨内皮迁移途径和B细胞信号传导受体途径有关的因子。值得注意的是lyn和pi3k的转录下调,这些分子已知与CD79A相互作用并控制B细胞受体信号传导过程。总之,这些结果突出了钩虫分泌的蛋白质与B细胞之间以前未知的相互作用,这对蠕虫驱动的免疫调节和疫苗开发具有影响。此外,人类蛋白质微阵列用于鉴定宿主-病原体相互作用的新颖用途,再加上离体结合研究和人类宿主细胞中全局基因表达的后续分析,展示了探索传染病分子基础的新途径。

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