Chengfeng Xia scite author profile

The development and maturation of semi-invariant natural killer T cells (iNKT cells) rely on the recognition of self antigens presented by CD1d restriction molecules in thymus. The nature of the stimulatory thymic self lipids remains elusive. We isolated lipids from thymocytes and found that ether-bonded mono-alkyl glycerophosphates and the precursors and degradation products of plasmalogens stimulated iNKT cells. Synthetic analogs showed high potency in activating thymic and peripheral iNKT cells. Mice deficient in the peroxisomal enzyme glyceronephosphate O-acyltransferase (GNPAT), essential for the synthesis of ether lipids, had significant alteration of the thymic maturation of iNKT cells and fewer iNKT cells in both thymus and peripheral organs, which confirmed the role of ether-bonded lipids as iNKT cell antigens. Thus, peroxisome-derived lipids are nonredundant self antigens required for the generation of a full iNKT cell repertoire.

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Remodeling bacterial polysaccharides by metabolic pathway engineering

Liu

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

108

114

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Introducing structural modifications into biomolecules represents a powerful approach to dissect their functions and roles in biological processes. Bacterial polysaccharides, despite their rich structural information and essential roles in bacterium-host interactions and bacterial virulence, have largely been unexplored for in vivo structural modifications. In this study, we demonstrate the incorporation of a panel of monosaccharide analogs into bacterial polysaccharides in a highly homogenous manner via metabolic engineering of a promiscuous sugar nucleotide biosynthetic pathway. In addition, the bioorthorgonal functional groups metabolically incorporated were exploited for cell surface labeling using in vitro selective chemical ligation reactions. In summary, our study presents a general, facile and effective approach for in vivo generation of novel tailor-made bacterial polysaccharides.chemical remodeling ͉ metabolic engineering ͉ sugar nucleotide biosynthesis ͉ fucose

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A novel self-lipid antigen targets human T cells against CD1c+ leukemias

Lepore¹,

Lalla

Gundimeda

et al. 2014

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Chengfeng Xia

Peroxisome-derived lipids are self antigens that stimulate invariant natural killer T cells in the thymus

Remodeling bacterial polysaccharides by metabolic pathway engineering

A novel self-lipid antigen targets human T cells against CD1c+ leukemias

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