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真皮含有朗格素阳性树突状细胞,其发育和功能独立于表皮朗格汉斯细胞。

The dermis contains langerin+ dendritic cells that develop and function independently of epidermal Langerhans cells.

作者信息

Poulin Lionel Franz, Henri Sandrine, de Bovis Béatrice, Devilard Elisabeth, Kissenpfennig Adrien, Malissen Bernard

机构信息

Centre d'Immunologie de Marseille-Luminy, Université de la Méditerrannée, Case 906, 13288 Marseille Cedex 9, France.

出版信息

J Exp Med. 2007 Dec 24;204(13):3119-31. doi: 10.1084/jem.20071724. Epub 2007 Dec 17.

Abstract

Langerhans cells (LCs) constitute a subset of dendritic cells (DCs) that express the lectin langerin and that reside in their immature state in epidermis. Paradoxically, in mice permitting diphtheria toxin (DT)-mediated ablation of LCs, epidermal LCs reappeared with kinetics that lagged behind that of their putative progeny found in lymph nodes (LNs). Using bone marrow (BM) chimeras, we showed that a major fraction of the langerin(+), skin-derived DCs found in LNs originates from a developmental pathway that is independent from that of epidermal LCs. This pathway, the existence of which was unexpected, originates in the dermis and gives rise to langerin(+) dermal DCs (DDCs) that should not be confused with epidermal LCs en route to LNs. It explains that after DT treatment, some langerin(+), skin-derived DCs reappear in LNs long before LC-derived DCs. Using CD45 expression and BrdU-labeling kinetics, both LCs and langerin(+) DDCs were found to coexist in wild-type mice. Moreover, DT-mediated ablation of epidermal LCs opened otherwise filled niches and permitted repopulation of adult noninflammatory epidermis with BM-derived LCs. Our results stress that the langerin(+) DC network is more complex than originally thought and have implications for the development of transcutaneous vaccines and the improvement of humanized mouse models.

摘要

朗格汉斯细胞(LCs)是树突状细胞(DCs)的一个亚群,表达凝集素朗格蛋白,并以未成熟状态存在于表皮中。矛盾的是,在允许白喉毒素(DT)介导消融LCs的小鼠中,表皮LCs重新出现的动力学滞后于其在淋巴结(LNs)中假定后代的动力学。利用骨髓(BM)嵌合体,我们发现淋巴结中发现的大部分朗格蛋白阳性、皮肤来源的DCs起源于一条独立于表皮LCs的发育途径。这条途径的存在出人意料,它起源于真皮,产生朗格蛋白阳性真皮DCs(DDCs),不应将其与前往淋巴结途中的表皮LCs混淆。这解释了DT治疗后,一些朗格蛋白阳性、皮肤来源的DCs在源自LCs的DCs之前很久就在淋巴结中重新出现。利用CD45表达和BrdU标记动力学,发现LCs和朗格蛋白阳性DDCs在野生型小鼠中共存。此外,DT介导的表皮LCs消融打开了原本被占据的生态位,并允许成年非炎症性表皮被源自BM的LCs重新填充。我们的结果强调,朗格蛋白阳性DC网络比最初认为的更复杂,对经皮疫苗的开发和人源化小鼠模型的改进具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/de65/2150992/e37e38cbcf5d/jem2043119f01.jpg

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