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Recent "glycolipids" articles

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Specific glycosphingolipids mediate epithelial-to-mesenchymal transition of human and mouse epithelial cell lines.
Feng Guan, Kazuko Handa, and Sen-itiroh Hakomori
Proceedings of the National Academy of Sciences of the United States of America 106 (18), 7461-6 (05 May 2009)
Posted by FGG and 1 other to 2009-May Glycolipids Development on Fri May 08 2009 at 15:56 UTC | info | related
 
Analysis of lectin binding to glycolipid complexes using combinatorial glycoarrays.
Simon Rinaldi et al.
Glycobiology, (06 Apr 2009)
Posted by FGG to 2009-May Glycolipids Techniques on Wed Apr 22 2009 at 12:32 UTC | info | related
 
Reducing glycosphingolipid content in adipose tissue of obese mice restores insulin sensitivity, adipogenesis and reduces inflammation.
Marco van Eijk et al.
PLoS ONE 4 (3), e4723 (2009)
Posted by FGG to 2009-Apr Glycolipids mouse Disease on Wed Mar 25 2009 at 13:30 UTC | info | related
 
Expression of ceramide glucosyltransferases, which are essential for glycosphingolipid synthesis, is only required in a small subset of C. elegans cells.
Esther Marza et al.
Journal of cell science 122 (Pt 6), 822-33 (15 Mar 2009)
 
Hybrid glycopeptide antibiotics
B Sun et al.
Journal of the American Chemical Society 123 (50), 12722-3 (19 Dec 2001)
 
Immunological-based assay methods for glycosyltransferase enzymes
L M Keshvara, S Gosselin, and M M Palcic
Glycobiology 3 (5), 416-8 (Oct 1993)
 
Structural dissection and high-throughput screening of mannosylglycerate synthase
James Flint et al.
Nature structural & molecular biology 12 (7), 608-14 (Jul 2005)
 
Two proteins homologous to the N- and C-terminal domains of the bacterial glycosyltransferase Murg are required for the second step of dolichyl-linked oligosaccharide synthesis in Saccharomyces cerevisiae
Isabelle Chantret et al.
The Journal of biological chemistry 280 (10), 9236-42 (11 Mar 2005)
 
Glycolipids of acid-fast bacteria.
E LEDERER
Advances in carbohydrate chemistry 16, 207-38 (1961)
 
CD1d-lipid-antigen recognition by the semi-invariant NKT T-cell receptor
Natalie Borg et al.
Nature 448 (7149), 44-9 (05 Jul 2007)
The CD1 family is a large cluster of non-polymorphic, major histocompatibility complex (MHC) class-I-like molecules that bind distinct lipid-based antigens that are recognized by T cells. The most studied group of T cells that interact with lipid antigens are natural killer T (NKT) cells, which characteristically express a semi-invariant T-cell receptor (NKT TCR) that specifically recognizes the CD1 family member, CD1d. NKT-cell-mediated recognition of the CD1d–antigen complex has been implicated in microbial immunity, tumour immunity, autoimmunity and allergy. Here we describe the structure of a human NKT TCR in complex with CD1d bound to the potent NKT-cell agonist alpha-galactosylceramide, the archetypal CD1d-restricted glycolipid. In contrast to T-cell receptor–peptide-antigen–MHC complexes, the NKT TCR docked parallel to, and at the extreme end of the CD1d-binding cleft, which enables a lock-and-key type interaction with the lipid antigen. The structure provides a basis for the interaction between the highly conserved NKT TCR alpha-chain and the CD1d–antigen complex that is typified in innate immunity, and also indicates how variability of the NKT TCR beta-chain can impact on recognition of other CD1d–antigen complexes. These findings provide direct insight into how a T-cell receptor recognizes a lipid-antigen-presenting molecule of the immune system.

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