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树突状细胞在人类生命周期中呈现出亚群和组织特异性的成熟动态。

Dendritic Cells Display Subset and Tissue-Specific Maturation Dynamics over Human Life.

作者信息

Granot Tomer, Senda Takashi, Carpenter Dustin J, Matsuoka Nobuhide, Weiner Joshua, Gordon Claire L, Miron Michelle, Kumar Brahma V, Griesemer Adam, Ho Siu-Hong, Lerner Harvey, Thome Joseph J C, Connors Thomas, Reizis Boris, Farber Donna L

机构信息

Columbia Center for Translational Immunology, Columbia University Medical Center, New York, NY 10032, USA; Department of Medicine, Columbia University Medical Center, New York, NY 10032, USA.

Columbia Center for Translational Immunology, Columbia University Medical Center, New York, NY 10032, USA; Department of Surgery, Columbia University Medical Center, New York, NY 10032, USA.

出版信息

Immunity. 2017 Mar 21;46(3):504-515. doi: 10.1016/j.immuni.2017.02.019.

Abstract

Maturation and migration to lymph nodes (LNs) constitutes a central paradigm in conventional dendritic cell (cDC) biology but remains poorly defined in humans. Using our organ donor tissue resource, we analyzed cDC subset distribution, maturation, and migration in mucosal tissues (lungs, intestines), associated lymph nodes (LNs), and other lymphoid sites from 78 individuals ranging from less than 1 year to 93 years of age. The distribution of cDC1 (CD141CD13) and cDC2 (Sirp-αCD1c) subsets was a function of tissue site and was conserved between donors. We identified cDC2 as the major mature (HLA-DR) subset in LNs with the highest frequency in lung-draining LNs. Mature cDC2 in mucosal-draining LNs expressed tissue-specific markers derived from the paired mucosal site, reflecting their tissue-migratory origin. These distribution and maturation patterns were largely maintained throughout life, with site-specific variations. Our findings provide evidence for localized DC tissue surveillance and reveal a lifelong division of labor between DC subsets, with cDC2 functioning as guardians of the mucosa.

摘要

成熟并迁移至淋巴结是传统树突状细胞(cDC)生物学的核心模式,但在人类中仍未得到充分界定。利用我们的器官捐献者组织资源,我们分析了78名年龄从不到1岁至93岁个体的黏膜组织(肺、肠道)、相关淋巴结以及其他淋巴部位中cDC亚群的分布、成熟情况和迁移情况。cDC1(CD141⁺CD13⁻)和cDC2(Sirp-α⁺CD1c⁺)亚群的分布是组织部位的函数,并且在捐献者之间是保守的。我们确定cDC2是淋巴结中主要的成熟(HLA-DR⁺)亚群,在肺引流淋巴结中频率最高。黏膜引流淋巴结中的成熟cDC2表达源自配对黏膜部位的组织特异性标志物,反映了它们的组织迁移起源。这些分布和成熟模式在一生中基本保持,存在部位特异性差异。我们的研究结果为局部树突状细胞组织监测提供了证据,并揭示了树突状细胞亚群之间终身的分工,其中cDC2作为黏膜的守护者发挥作用。

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