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用于小鼠 NKT 细胞的多种内源性抗原:非糖脂的自身抗原。

Diverse endogenous antigens for mouse NKT cells: self-antigens that are not glycosphingolipids.

机构信息

Division of Developmental Immunology, La Jolla Institute for Allergy and Immunology, La Jolla, CA 92037, USA.

出版信息

J Immunol. 2011 Feb 1;186(3):1348-60. doi: 10.4049/jimmunol.1001008. Epub 2010 Dec 29.

Abstract

NKT cells with an invariant Ag receptor (iNKT cells) represent a highly conserved and unique subset of T lymphocytes having properties of innate and adaptive immune cells. They have been reported to regulate a variety of immune responses, including the response to cancers and the development of autoimmunity. The development and activation of iNKT cells is dependent on self-Ags presented by the CD1d Ag-presenting molecule. It is widely believed that these self-Ags are glycosphingolipids (GSLs), molecules that contain ceramide as the lipid backbone. In this study, we used a variety of methods to show that mammalian Ags for mouse iNKT cells need not be GSLs, including the use of cell lines deficient in GSL biosynthesis and an inhibitor of GSL biosynthesis. Presentation of these Ags required the expression of CD1d molecules that could traffic to late endosomes, the site where self-Ag is acquired. Extracts of APCs contain a self-Ag that could stimulate iNKT cells when added to plates coated with soluble, rCD1d molecules. The Ag(s) in these extracts are resistant to sphingolipid-specific hydrolase digestion, consistent with the results using live APCs. Lyosphosphatidylcholine, a potential self-Ag that activated human iNKT cell lines, did not activate mouse iNKT cell hybridomas. Our data indicate that there may be more than one type of self-Ag for iNKT cells, that the self-Ags comparing mouse and human may not be conserved, and that the search to identify these molecules should not be confined to GSLs.

摘要

NKT 细胞具有不变的 Ag 受体(iNKT 细胞),代表了具有先天和适应性免疫细胞特性的高度保守和独特的 T 淋巴细胞亚群。据报道,它们可以调节多种免疫反应,包括对癌症的反应和自身免疫的发展。iNKT 细胞的发育和激活依赖于由 CD1d Ag 呈递分子呈递的自身 Ag。人们普遍认为这些自身 Ag 是糖脂 (GSLs),是含有神经酰胺作为脂质主链的分子。在这项研究中,我们使用了多种方法来表明,用于小鼠 iNKT 细胞的哺乳动物 Ag 不一定是 GSLs,包括使用缺乏 GSL 生物合成的细胞系和 GSL 生物合成抑制剂。这些 Ag 的呈递需要表达能够转运到晚期内体的 CD1d 分子,晚期内体是获得自身 Ag 的部位。APCs 的提取物中含有一种 Ag,当添加到用可溶性 rCD1d 分子包被的平板上时,这种 Ag 可以刺激 iNKT 细胞。这些提取物中的 Ag(s) 对鞘脂特异性水解酶具有抗性,这与使用活 APCs 的结果一致。溶血磷脂胆碱是一种潜在的激活人 iNKT 细胞系的自身 Ag,但不能激活小鼠 iNKT 细胞杂交瘤。我们的数据表明,iNKT 细胞可能有不止一种自身 Ag,比较小鼠和人类的自身 Ag 可能不保守,并且不应将这些分子的搜索仅限于 GSLs。

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