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Dual effect of Thymosin α 1 on human monocyte-derived dendritic cellin vitrostimulated with viral and bacterial toll-like receptor agonists

机译:胸腺素α1对人单核细胞衍生的树突状纤维菌素的双重作用,病毒和细菌性收缩受体激动剂

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摘要

OBJECTIVES:udThymosin α 1 (Tα1) recently gained interest as immune adjuvant for vaccines because of its ability to modulate the T-cell/dendritic cell (DC) axis and to improve antibody production. The objective of this study was to determine whether Tα1 would address in vitro the response of human primary monocyte-derived DC, crucial regulators of vaccine-induced immunity, upon exposure to different toll-like receptor (TLR) agonists or infection with viruses or bacteria.udMETHODS:udDC maturation and production of pro-inflammatory cytokines were analyzed.udRESULTS:udOur data revealed a dual effect of Tα1 on DC biology upon viral or bacterial stimulation. Interestingly, Tα1 enhanced human leukocyte antigen (HLA)-I and II surface expression and secretion of IL-6, TNF-α and IL-8 when DCs were treated with viral TLR3 and TLR7/8 agonists. Similarly, in pandemic H1N1 influenza A-infected DCs, Tα1 raised the expression of maturation markers and type I and III Interferon (IFN). In contrast, following bacterial TLR2 and 4 stimulation, as well as upon Bacillus Calmette-Guerin infection, the presence of Tα1 in DC cultures drastically lowered the analyzed cellular parameters.udCONCLUSION:udThe knowledge that Tα1 pleiotropic effect might ameliorate anti-viral immune responses and, at the same time, dampen inflammation caused by bacterial infections could lay the groundwork for a more appropriate therapeutic application of this molecule.
机译:目的:udthymosinα1(tα1)最近获得了疫苗的免疫佐剂,因为它能够调节T细胞/树突细胞(DC)轴并改善抗体产生。本研究的目的是确定Tα1是否会在体外解决人初级单核细胞衍生的DC,疫苗诱导的免疫病的关键调节因子,在暴露于不同的收费(TLR)激动剂或用病毒或细菌感染时。 udmethods: UDDC成熟和促炎细胞因子的成熟和生产。 Udresults: Udour数据在病毒或细菌刺激时揭示了Tα1对DC生物学的双重影响。有趣的是,当DC用病毒TLR3和TLR7 / 8激动剂处理DC时,Tα1增强的人白细胞抗原(HLA)-I和II表面表达和II表面表达和II-6,TNF-α和IL-8的分泌。类似地,在大流行的H1N1流感A感染的DC中,Tα1提出了成熟标志物和I型和III干扰素(IFN)的表达。相比之下,在细菌TLR2和4刺激之后,以及芽孢杆菌均匀引导感染,DC培养物中的Tα1的存在急剧降低了分析的细胞参数。 Udconclusion: Ud知道Tα1脂肪效应可能改善抗病毒免疫反应和同时,由细菌感染引起的抑制炎症可以为该分子进行更适当的治疗施用来奠定基础。

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