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稳态及感染期间的派尔集合淋巴结单核吞噬细胞系统

The Peyer's Patch Mononuclear Phagocyte System at Steady State and during Infection.

作者信息

Da Silva Clément, Wagner Camille, Bonnardel Johnny, Gorvel Jean-Pierre, Lelouard Hugues

机构信息

Aix-Marseille University, CNRS, INSERM, CIML, Marseille, France.

Laboratory of Myeloid Cell Ontogeny and Functional Specialisation, VIB Inflammation Research Center, Ghent, Belgium.

出版信息

Front Immunol. 2017 Oct 2;8:1254. doi: 10.3389/fimmu.2017.01254. eCollection 2017.

Abstract

The gut represents a potential entry site for a wide range of pathogens including protozoa, bacteria, viruses, or fungi. Consequently, it is protected by one of the largest and most diversified population of immune cells of the body. Its surveillance requires the constant sampling of its encounters by dedicated sentinels composed of follicles and their associated epithelium located in specialized area. In the small intestine, Peyer's patches (PPs) are the most important of these mucosal immune response inductive sites. Through several mechanisms including transcytosis by specialized epithelial cells called M-cells, access to the gut lumen is facilitated in PPs. Although antigen sampling is critical to the initiation of the mucosal immune response, pathogens have evolved strategies to take advantage of this permissive gateway to enter the host and disseminate. It is, therefore, critical to decipher the mechanisms that underlie both host defense and pathogen subversive strategies in order to develop new mucosal-based therapeutic approaches. Whereas penetration of pathogens through M cells has been well described, their fate once they have reached the subepithelial dome (SED) remains less well understood. Nevertheless, it is clear that the mononuclear phagocyte system (MPS) plays a critical role in handling these pathogens. MPS members, including both dendritic cells and macrophages, are indeed strongly enriched in the SED, interact with M cells, and are necessary for antigen presentation to immune effector cells. This review focuses on recent advances, which have allowed distinguishing the different PP mononuclear phagocyte subsets. It gives an overview of their diversity, specificity, location, and functions. Interaction of PP phagocytes with the microbiota and the follicle-associated epithelium as well as PP infection studies are described in the light of these new criteria of PP phagocyte identification. Finally, known alterations affecting the different phagocyte subsets during PP stimulation or infection are discussed.

摘要

肠道是包括原生动物、细菌、病毒或真菌在内的多种病原体的潜在入侵部位。因此,它受到体内最大且最多样化的免疫细胞群体之一的保护。其监测需要由位于特定区域的滤泡及其相关上皮组成的专门哨兵不断对其接触物进行采样。在小肠中,派尔集合淋巴结(PPs)是这些黏膜免疫反应诱导部位中最重要的。通过几种机制,包括由称为M细胞的特殊上皮细胞进行转胞吞作用,PPs促进了对肠腔的 access。虽然抗原采样对于黏膜免疫反应的启动至关重要,但病原体已经进化出利用这个宽松通道进入宿主并传播的策略。因此,解读宿主防御和病原体颠覆策略背后的机制对于开发新的基于黏膜的治疗方法至关重要。虽然病原体通过M细胞的穿透已经得到了很好的描述,但它们到达上皮下圆顶(SED)后的命运仍不太清楚。然而,很明显单核吞噬细胞系统(MPS)在处理这些病原体方面起着关键作用。MPS成员,包括树突状细胞和巨噬细胞,确实在SED中高度富集,与M细胞相互作用,并且对于向免疫效应细胞呈递抗原是必需的。本综述重点关注最近的进展,这些进展有助于区分不同的PP单核吞噬细胞亚群。它概述了它们的多样性、特异性、位置和功能。根据这些新的PP吞噬细胞识别标准,描述了PP吞噬细胞与微生物群和滤泡相关上皮的相互作用以及PP感染研究。最后,讨论了在PP刺激或感染期间影响不同吞噬细胞亚群的已知改变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e91c/5630697/bf5639137d93/fimmu-08-01254-g001.jpg

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