Literature DB >> 22917572

Ganglioside-binding specificities of E. coli enterotoxin LT-IIc: Importance of long-chain fatty acyl ceramide.

Charles S Berenson1, Hesham F Nawar, Ragina L Kruzel, Lorrie M Mandell, Terry D Connell.   

Abstract

Bacterial heat-labile (LT) enterotoxins signal through tightly regulated interactions with host cell gangliosides. LT-IIa and LT-IIb of Escherichia coli bind preferentially to gangliosides with a NeuAcα2-3Galβ1-3GalNAc terminus, with key distinctions in specificity. LT-IIc, a newly discovered E. coli LT, is comprised of an A polypeptide with high homology, and a B polypeptide with moderate homology, to LT-IIa and LT-IIb. LT-IIc is less cytotoxic than LT-IIa and LT-IIb. We theorized that LT-IIc-host cell interaction is regulated by specific structural attributes of immune cell ganglioside receptors and designed experiments to test this hypothesis. Overlay immunoblotting to a diverse array of neural and macrophage gangliosides indicated that LT-IIc bound to a restrictive range of gangliosides, each possessing a NeuAcα2-3Galβ1-3GalNAc with a requisite terminal sialic acid. LT-IIc did not bind to GM1a with short-chain fatty acyl ceramides. Affinity overlay immunoblots, constructed to a diverse array of known ganglioside structures of murine peritoneal macrophages, established that LT-IIc bound to GM1a comprised of long-chain fatty acyl ceramides. Findings were confirmed with LT-IIc also binding to GM1a of RAW264.7 cells, comprised of a long-chain fatty acyl ceramide. Thus, LT-IIc-ganglioside binding differs distinctly from that of LT-IIa and LT-IIb. LT-IIc binding is not just dependent on carbohydrate composition, but also upon the orientation of the oligosaccharide portion of GM1a by the ceramide moiety. These studies are the first demonstration of LT-ganglioside dependence upon ceramide composition and underscore the contribution of long-chain fatty acyl ceramides to host cell interactions.

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Year:  2012        PMID: 22917572      PMCID: PMC3505011          DOI: 10.1093/glycob/cws123

Source DB:  PubMed          Journal:  Glycobiology        ISSN: 0959-6658            Impact factor:   4.313


  32 in total

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Authors:  J C Osborne; J Moss; P H Fishman; S Nakaya; D C Robertson
Journal:  Biophys J       Date:  1982-01       Impact factor: 4.033

2.  Chemiluminescence detection of gangliosides by thin-layer chromatography.

Authors:  S L Arnsmeier; A S Paller
Journal:  J Lipid Res       Date:  1995-04       Impact factor: 5.922

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Authors:  V Bennett; P Cuatrecasas
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Review 4.  Evidence that molecules on the surface of one cell can adhere to the oligosaccharide portion of gangliosides on the surface of another cell.

Authors:  C L Schengrund
Journal:  Biol Signals       Date:  1995 Jan-Feb

Review 5.  Significance of glycosphingolipid fatty acid chain length on membrane microdomain-mediated signal transduction.

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Journal:  Glycoconj J       Date:  2007-11-28       Impact factor: 2.916

7.  LT-IIc, a new member of the type II heat-labile enterotoxin family encoded by an Escherichia coli strain obtained from a nonmammalian host.

Authors:  Hesham F Nawar; Natalie D King-Lyons; John C Hu; Raymond C Pasek; Terry D Connell
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8.  N-glycolyl GM1 ganglioside as a receptor for simian virus 40.

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9.  Mutational analysis of the ganglioside-binding activity of the type II Escherichia coli heat-labile enterotoxin LT-IIb.

Authors:  T D Connell; R K Holmes
Journal:  Mol Microbiol       Date:  1995-04       Impact factor: 3.501

10.  Type II heat-labile enterotoxins from 50 diverse Escherichia coli isolates belong almost exclusively to the LT-IIc family and may be prophage encoded.

Authors:  Michael G Jobling; Randall K Holmes
Journal:  PLoS One       Date:  2012-01-05       Impact factor: 3.240

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4.  Characterization of the ganglioside recognition profile of Escherichia coli heat-labile enterotoxin LT-IIc.

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Review 5.  Protein Toxins That Utilize Gangliosides as Host Receptors.

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6.  Enhancement of humoral immunity by the type II heat-labile enterotoxin LT-IIb is dependent upon IL-6 and neutrophils.

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Review 7.  The Many Facets of Sphingolipids in the Specific Phases of Acute Inflammatory Response.

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