首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Sequence independent interferon-alpha induction by multimerized phosphodiester DNA depends on spatial regulation of Toll-like receptor-9 activation in plasmacytoid dendritic cells.
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Sequence independent interferon-alpha induction by multimerized phosphodiester DNA depends on spatial regulation of Toll-like receptor-9 activation in plasmacytoid dendritic cells.

机译:多聚磷酸二酯DNA的序列无关干扰素α诱导取决于浆细胞样树突状细胞中Toll样受体9激活的空间调节。

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摘要

Single-stranded versus multimeric phosphorothioate-modified CpG oligodeoxynucleotides (ODNs) undergo differential endosomal trafficking upon uptake into plasmacytoid dendritic cells (pDCs), correlating with Toll-like receptor-9-dependent pDC maturation/activation (single-stranded B-type CpG ODN) or interferon-alpha (IFN-alpha) induction (multimeric A-type CpG ODN), respectively. As was recently shown, IFN-alpha production, other than by CpG ODNs, can also be induced in a sequence-independent manner by phosphodiester (PD) ODNs multimerized by 3' poly-guanosine (poly-G) tails. We investigate here the type of endosomal trafficking responsible for IFN-alpha induction by natural PD ODN ligands. We show that 3' extension with poly-G tails leads to multimerization of single-stranded PD ODNs and to enhanced cellular uptake into pDCs. While monomeric PD ODNs, which induce CpG-dependent Toll-like receptor-9 stimulation and pDC maturation/activation, localized to late endosomal/lysosomal compartments, the poly-G multimerized PD ODNs, which induce CpG-independent IFN-alpha production, located to vesicles with a distinct, 'early' endosomal phenotype. We conclude that poly-G-mediated multimerization of natural PD ODNs allows for sequence-independent, Toll-like receptor-9-dependent IFN-alpha induction in pDCs by combining three distinct effects: relative protection of sensitive PD ODNs from extracellular and intracellular DNase degradation, enhanced cellular uptake and preferential early endosomal compartmentation.
机译:单链或多聚硫代磷酸酯修饰的CpG寡脱氧核苷酸(ODN)在摄入浆细胞样树突状细胞(pDC)后经历了不同的内体运输,与Toll样受体9依赖性pDC成熟/激活相关(单链B型CpG ODN) )或干扰素-α(IFN-α)诱导(多聚A型CpG ODN)。如最近所显示的,除了CpG ODN以外,IFN-α的产生还可以通过与3'聚鸟苷(poly-G)尾部多聚的磷酸二酯(PD)ODN以序列独立的方式诱导。我们在这里调查负责通过天然PD ODN配体诱导IFN-α的内体运输类型。我们显示,具有聚G尾巴的3'延伸导致单链PD ODN的多聚化,并增强了细胞对pDC的摄取。单体PD ODNs定位于晚期的内体/溶酶体区室,它诱导CpG依赖的Toll样受体9刺激和pDC成熟/激活,而聚G多聚PD ODNs可以诱导不依赖CpG的IFN-α产生。具有明显的“早期”内体表型的囊泡。我们得出的结论是,通过结合三种不同的作用,p-DC中天然PD ODN的多G介导的多聚体允许序列独立,Toll样受体9依赖性IFN-α诱导:相对保护敏感PD ODN免受细胞外和细胞内DNase的影响降解,增强的细胞摄取和优先的早期内体间隔。

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