首页> 外文期刊>European Journal of Immunology >Essential role of Rip2 in the modulation of innate and adaptive immunity triggered by Nod1 and Nod2 ligands.
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Essential role of Rip2 in the modulation of innate and adaptive immunity triggered by Nod1 and Nod2 ligands.

机译:调制的Rip2先天的重要作用和适应性免疫Nod1和Nod2触发配体。

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摘要

Muramyl peptides are the building blocks of bacterial peptidoglycan, and their biological functions in mammals have been extensively studied. In particular, muramyl peptides trigger inflammation, contribute to host defense against microbial infections, and modulate the adaptive immune response to antigens. These bacterial molecules are detected by nucleotide oligomerization domain 1 (Nod1) and Nod2, and recent evidence suggests that muramyl dipeptide also activates NLRP3 and NLRP1 inflammasomes. Here, we investigated the role of Rip2, the adaptor for Nod1- and Nod2-dependent signaling, in multiple aspects of the host response to muramyl peptides in vivo, such as inflammatory cytokine secretion, activation and recruitment of macrophages and neutrophils to the site of injection, systemic activation of myeloid, T and B cells in the spleen, adjuvanticity and capacity to polarize the adaptive response to ovalbumin. Our results demonstrate that Rip2 was crucial for all the biological functions studied. We also identified CD11c(int) CD11b(+) inflammatory dendritic cells as a major myeloid cell population responding to Nod stimulation in vivo. Together, our results highlight the importance of Rip2 for Nod-dependent induction of innate and adaptive immunity.
机译:胞壁肽的基石细菌肽聚糖,和他们的生物在哺乳动物中都进行了广泛的功能研究。炎症,导致主机防御微生物感染和调节自适应免疫反应的抗原。由核苷酸分子检测寡聚化域1 (Nod1)和Nod2,最近的证据表明,胞壁二肽也激活NLRP3 NLRP1 inflammasomes。在这里,我们调查的角色Rip2,适配器为Nod1 Nod2-dependent信号,在多个方面的回应胞壁肽在体内,如炎症细胞因子分泌,激活和招聘巨噬细胞和中性粒细胞的网站注入,系统性激活的骨髓,T和B细胞在脾脏,adjuvanticity和能力去极化卵白蛋白的适应性反应。我们的研究结果表明,Rip2至关重要所有的生物功能研究。确定CD11c (int) CD11b(+)炎症树突状细胞作为主要的骨髓细胞人口应对点头刺激体内。在一起,我们的研究结果强调的重要性Rip2 Nod-dependent感应的先天适应性免疫。

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