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巨噬细胞炎性蛋白3α参与表皮朗格汉斯细胞的组成型运输。

Macrophage inflammatory protein 3alpha is involved in the constitutive trafficking of epidermal langerhans cells.

作者信息

Charbonnier A S, Kohrgruber N, Kriehuber E, Stingl G, Rot A, Maurer D

机构信息

Division of Immunology, Department of Dermatology, University of Vienna Medical School, A-1090 Vienna, Austria.

出版信息

J Exp Med. 1999 Dec 20;190(12):1755-68. doi: 10.1084/jem.190.12.1755.

Abstract

Certain types of dendritic cells (DCs) appear in inflammatory lesions of various etiologies, whereas other DCs, e.g., Langerhans cells (LCs), populate peripheral organs constitutively. Until now, the molecular mechanism behind such differential behavior has not been elucidated. Here, we show that CD1a(+) LC precursors respond selectively and specifically to the CC chemokine macrophage inflammatory protein (MIP)-3alpha. In contrast, CD14(+) precursors of DC and monocytes are not attracted by MIP-3alpha. LCs lose the migratory responsiveness to MIP-3alpha during their maturation, and non-LC DCs do not acquire MIP-3alpha sensitivity. The notion that MIP-3alpha may be responsible for selective LC recruitment into the epidermis is further supported by the following observations: (a) MIP-3alpha is expressed by keratinocytes and venular endothelial cells in clinically normal appearing human skin; (b) LCs express CC chemokine receptor (CCR)6, the sole MIP-3alpha receptor both in situ and in vitro; and (c) non-LC DCs that are not found in normal epidermis lack CCR6. The mature forms of LCs and non-LC DCs display comparable sensitivity for MIP-3beta, a CCR7 ligand, suggesting that DC subtype-specific chemokine responses are restricted to the committed precursor stage. Although LC precursors express primarily CCR6, non-LC DC precursors display a broad chemokine receptor repertoire. These findings reflect a scenario where the differential expression of chemokine receptors by two different subpopulations of DCs determines their functional behavior. One type, the LC, responds to MIP-3alpha and enters skin to screen the epidermis constitutively, whereas the other type, the "inflammatory" DC, migrates in response to a wide array of different chemokines and is involved in the amplification and modulation of the inflammatory tissue response.

摘要

某些类型的树突状细胞(DC)出现在各种病因的炎症病变中,而其他DC,如朗格汉斯细胞(LC),则持续存在于外周器官中。到目前为止,这种差异行为背后的分子机制尚未阐明。在此,我们表明CD1a(+) LC前体细胞对CC趋化因子巨噬细胞炎性蛋白(MIP)-3α有选择性和特异性反应。相比之下,DC和单核细胞的CD14(+)前体细胞不受MIP-3α吸引。LC在成熟过程中失去对MIP-3α的迁移反应性,而非LC DC则不会获得MIP-3α敏感性。以下观察结果进一步支持了MIP-3α可能负责将LC选择性募集到表皮中的观点:(a)MIP-3α由临床外观正常的人类皮肤中的角质形成细胞和小静脉内皮细胞表达;(b)LC表达CC趋化因子受体(CCR)6,这是原位和体外唯一的MIP-3α受体;(c)在正常表皮中未发现的非LC DC缺乏CCR6。LC和非LC DC的成熟形式对CCR7配体MIP-3β表现出相当的敏感性,这表明DC亚型特异性趋化因子反应仅限于定向前体细胞阶段。尽管LC前体细胞主要表达CCR6,但非LC DC前体细胞表现出广泛的趋化因子受体谱。这些发现反映了一种情况,即DC的两个不同亚群趋化因子受体的差异表达决定了它们的功能行为。一种类型,即LC,对MIP-3α作出反应并进入皮肤以持续筛选表皮,而另一种类型,即“炎性”DC,则对多种不同趋化因子作出反应并参与炎症组织反应的放大和调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7331/2195721/f76a83f9775a/JEM991262.f1.jpg

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