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NKG2D配体的急性上调促进局部免疫区室的快速重组,对肿瘤发生具有多效性作用。

Acute upregulation of an NKG2D ligand promotes rapid reorganization of a local immune compartment with pleiotropic effects on carcinogenesis.

作者信息

Strid Jessica, Roberts Scott J, Filler Renata B, Lewis Julia M, Kwong Bernice Y, Schpero William, Kaplan Daniel H, Hayday Adrian C, Girardi Michael

机构信息

Peter Gorer Department of Immunobiology, King's College London School of Medicine at Guy's Hospital, London SE1 9RT, UK.

出版信息

Nat Immunol. 2008 Feb;9(2):146-54. doi: 10.1038/ni1556. Epub 2008 Jan 6.

Abstract

The self-encoded ligands MICA (human) and Rae-1 (mouse) for the cytotoxic lymphocyte activating receptor NKG2D are highly expressed in carcinomas and inflammatory lesions and have been linked to immunosurveillance and graft rejection. However, whether NKG2D ligands have an intrinsic ability to acutely regulate tissue-associated immune compartments is not known. Here we show that epidermis-specific upregulation of Rae-1 induced rapid, coincident and reversible changes in the organization of tissue-resident V(gamma)5V(delta)1 TCRgammadelta+ intraepithelial T cells and Langerhans cells, swiftly followed by epithelial infiltration by unconventional alphabeta T cells. Whereas local V(gamma)5V(delta)1+ T cells limited carcinogenesis, Langerhans cells unexpectedly promoted it. These results provide unique insight into the early phases of tissue immunosurveillance and indicate that acute changes in NKG2D ligands may alone initiate a rapid, multifaceted immunosurveillance response in vivo.

摘要

细胞毒性淋巴细胞激活受体NKG2D的自身编码配体MICA(人类)和Rae-1(小鼠)在癌组织和炎性病变中高度表达,并与免疫监视和移植排斥相关。然而,NKG2D配体是否具有急性调节组织相关免疫区室的内在能力尚不清楚。在此我们表明,Rae-1在表皮特异性上调可诱导组织驻留的V(γ)5V(δ)1 TCRγδ+上皮内T细胞和朗格汉斯细胞的组织迅速、同时且可逆地发生变化,随后非常规αβ T细胞迅速浸润上皮。虽然局部V(γ)5V(δ)1+ T细胞可限制致癌作用,但朗格汉斯细胞却意外地促进了致癌作用。这些结果为组织免疫监视的早期阶段提供了独特的见解,并表明NKG2D配体的急性变化可能单独在体内引发快速、多方面的免疫监视反应。

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