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CD1 脂质组揭示了脂质结合基序和基于大小的抗原展示机制。

CD1 lipidomes reveal lipid-binding motifs and size-based antigen-display mechanisms.

机构信息

Division of Rheumatology, Immunity and Inflammation, Brigham and Women's Hospital, Harvard Medical School, Boston, MA 02115, USA.

Infection and Immunity Program and Department of Biochemistry and Molecular Biology, Biomedicine Discovery Institute, Monash University, Clayton, VIC 3800, Australia; Australian Research Council Centre of Excellence for Advanced Molecular Imaging, Monash University, Clayton, VIC 3800, Australia.

出版信息

Cell. 2023 Oct 12;186(21):4583-4596.e13. doi: 10.1016/j.cell.2023.08.022. Epub 2023 Sep 18.

Abstract

The CD1 system binds lipid antigens for display to T cells. Here, we solved lipidomes for the four human CD1 antigen-presenting molecules, providing a map of self-lipid display. Answering a basic question, the detection of >2,000 CD1-lipid complexes demonstrates broad presentation of self-sphingolipids and phospholipids. Whereas peptide antigens are chemically processed, many lipids are presented in an unaltered form. However, each type of CD1 protein differentially edits the self-lipidome to show distinct capture motifs based on lipid length and chemical composition, suggesting general antigen display mechanisms. For CD1a and CD1d, lipid size matches the CD1 cleft volume. CD1c cleft size is more variable, and CD1b is the outlier, where ligands and clefts show an extreme size mismatch that is explained by uniformly seating two small lipids in one cleft. Furthermore, the list of compounds that comprise the integrated CD1 lipidome supports the ongoing discovery of lipid blockers and antigens for T cells.

摘要

CD1 系统结合脂质抗原以供 T 细胞呈递。在这里,我们解决了四种人类 CD1 抗原呈递分子的脂质组,提供了自我脂质呈递图谱。回答了一个基本问题,即检测到超过 2000 种 CD1-脂质复合物表明广泛呈现自身鞘脂和磷脂。虽然肽抗原是通过化学处理的,但许多脂质以未改变的形式呈现。然而,每种类型的 CD1 蛋白都以不同的方式编辑自我脂质组,根据脂质长度和化学组成显示出独特的捕获基序,这表明存在一般的抗原呈递机制。对于 CD1a 和 CD1d,脂质大小与 CD1 裂隙体积相匹配。CD1c 裂隙大小变化较大,而 CD1b 是例外,其配体和裂隙显示出极端的大小不匹配,这可以通过在一个裂隙中均匀地容纳两个小脂质来解释。此外,构成综合 CD1 脂质组的化合物列表支持正在发现的 T 细胞脂质阻滞剂和抗原。

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