Krumbiegel Doreen, Zepp Fred, Meyer Claudius Ullrich
Department of Pediatric Immunology, Children's Hospital, University of Mainz, Germany.
Hum Immunol. 2007 Oct;68(10):813-22. doi: 10.1016/j.humimm.2007.08.001. Epub 2007 Aug 29.
Dendritic cells (DC) are thought to be responsible for the reduced ability of human newborns to induce protective T-helper 1 (Th1) immune responses. The key player in Th1 differentiation, interleukin-12 (IL-12), is primarily produced in response to Toll-like receptor (TLR) binding by adult DC but not by neonatal DC. The potential use of various TLR agonist combinations for initiating neonatal monocyte-derived DC to prime Th1 responses was investigated. Single TLR ligands induced maturation only in adult DC; neonatal DC matured with combined targeting of TLR3/TLR8 or TLR4/TLR8, based on the expression of maturation markers. Similarly, the synergistic effects of combined TLR ligands could also be shown with adult and neonatal cytokine production, but different expression patterns were noted. In particular, IL-12p70 was produced by neonatal DC exclusively after combined TLR stimulation. Surprisingly, it was found that supernatants of combined stimulated neonatal DC could induce interferon-gamma production in autologous naïve T cells. Moreover, this interferon-gamma secretion was blocked by anti-IL-12p70 antibodies and increased after addition of recombined IL-12. In conclusion, these findings underline the differences between adult and neonatal DC and might suggest new strategies for promoting newborn Th1 immunity in response to pathogens and vaccine antigens.
树突状细胞(DC)被认为是导致人类新生儿诱导保护性辅助性T细胞1(Th1)免疫反应能力降低的原因。Th1分化的关键因子白细胞介素-12(IL-12)主要是成年DC在Toll样受体(TLR)结合后产生的,而新生儿DC则不会产生。研究了各种TLR激动剂组合用于启动新生儿单核细胞衍生DC引发Th1反应的潜在用途。单一TLR配体仅能诱导成年DC成熟;基于成熟标志物的表达,新生儿DC在TLR3/TLR8或TLR4/TLR8联合靶向作用下成熟。同样,联合TLR配体的协同效应在成年和新生儿细胞因子产生方面也有所体现,但观察到了不同的表达模式。特别是,新生儿DC仅在联合TLR刺激后产生IL-12p70。令人惊讶的是,发现联合刺激的新生儿DC的上清液可诱导自体幼稚T细胞产生干扰素-γ。此外,这种干扰素-γ分泌被抗IL-12p70抗体阻断,添加重组IL-12后分泌增加。总之,这些发现突出了成年和新生儿DC之间的差异,并可能为促进新生儿针对病原体和疫苗抗原的Th1免疫提出新策略。
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