SARS 刺突蛋白诱导人 B 细胞向巨噬样细胞的表型转化。
SARS spike protein induces phenotypic conversion of human B cells to macrophage-like cells.
机构信息
Graduate Institute of Microbiology and Public Health, National Chung Hsing University, 250 Kuo Kuang Road, Taichung 40227, Taiwan.
出版信息
Mol Immunol. 2010 Oct;47(16):2575-86. doi: 10.1016/j.molimm.2010.06.014. Epub 2010 Jul 27.
Massive aggregations of macrophages are frequently detected in afflicted lungs of patients with severe acute respiratory syndrome-associated coronavirus (SARS-CoV) infection. In vitro, ectopic expression of transcription factors, in particular CCAAT/enhancer-binding protein alpha (C/EBPα) and C/EBPβ, can convert B cells into functional macrophages. However, little is known about the specific ligands responsible for such phenotype conversion. Here, we investigated whether spike protein of SARS-CoV can act as a ligand to trigger the conversion of B cells to macrophages. We transduced SARS-CoV spike protein-displayed recombinant baculovirus (SSDRB), vAtEpGS688, into peripheral B cells and B lymphoma cells. Cell surface expression of CD19 or Mac-1 (CD11b) was determined by flow cytometry. SSDRB-mediated changes in gene expression profiles of B lymphoma cells were analyzed by microarray. In this report, we showed that spike protein of SARS virus could induce phenotypic conversion of human B cells, either from peripheral blood or B lymphoma cells, to macrophage-like cells that were steadily losing the B-cell marker CD19 and in turn expressing the macrophage-specific marker Mac-1. Furthermore, we found that SSDRB enhanced the expression of CD86, hypoxia-inducible factor-1α (HIF1α), suppressor of cytokine signaling (SOCS or STAT-induced STAT inhibitor)-3, C/EBPβ, insulin-like growth factor-binding protein 3 (IGFBP3), Krüpple-like factor (KLF)-5, and CD54, without marked influence on C/EBPα or PU.1 expression in transduced cells. Prolonged exposure to hypoxia could also induce macrophage-like conversion of B cells. These macrophage-like cells were defective in phagocytosis of red fluorescent beads. In conclusion, our results suggest that conversion of B cells to macrophage-like cells, similar to a pathophysiological response, could be mediated by a devastating viral ligand, in particular spike protein of SARS virus, or in combination with severe local hypoxia, which is a condition often observed in afflicted lungs of SARS patients.
大量的巨噬细胞聚集物经常在严重急性呼吸综合征相关冠状病毒(SARS-CoV)感染患者的受影响肺部中被检测到。在体外,异位表达转录因子,特别是CCAAT/增强子结合蛋白α(C/EBPα)和 C/EBPβ,可以将 B 细胞转化为功能性巨噬细胞。然而,对于导致这种表型转化的特定配体知之甚少。在这里,我们研究了 SARS-CoV 的刺突蛋白是否可以作为配体触发 B 细胞向巨噬细胞的转化。我们将 SARS-CoV 刺突蛋白展示的重组杆状病毒(SSDRB)vAtEpGS688 转导到外周 B 细胞和 B 淋巴瘤细胞中。通过流式细胞术测定细胞表面 CD19 或 Mac-1(CD11b)的表达。通过微阵列分析 SSDRB 介导的 B 淋巴瘤细胞基因表达谱的变化。在本报告中,我们表明 SARS 病毒的刺突蛋白可以诱导人 B 细胞的表型转化,无论是来自外周血还是 B 淋巴瘤细胞,转化为巨噬样细胞,这些细胞稳定地失去 B 细胞标记物 CD19,转而表达巨噬细胞特异性标记物 Mac-1。此外,我们发现 SSDRB 增强了 CD86、缺氧诱导因子-1α(HIF1α)、细胞因子信号转导抑制物(SOCS 或 STAT 诱导的 STAT 抑制剂)-3、C/EBPβ、胰岛素样生长因子结合蛋白 3(IGFBP3)、Krüpple 样因子(KLF)-5 和 CD54 的表达,而对转导细胞中 C/EBPα 或 PU.1 的表达没有明显影响。长时间暴露于缺氧也可以诱导 B 细胞向巨噬样细胞转化。这些巨噬样细胞在吞噬红色荧光珠方面存在缺陷。总之,我们的结果表明,B 细胞向巨噬样细胞的转化类似于病理生理反应,可能由破坏性病毒配体介导,特别是 SARS 病毒的刺突蛋白,或与严重局部缺氧相结合,这是 SARS 患者受影响肺部中经常观察到的情况。
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