Pertussis toxin has eukaryotic-like carbohydrate recognition domains.

Saukkonen, Kirsi; Burnette, W N; Mar, V L; Masure, H R; Tuomanen, Elaine

doi:10.1073/pnas.89.1.118

Cited by 125 publications

(121 citation statements)

References 27 publications

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“…Both N-acetylneuramin-lactose (1 -80 pM) and the cerebroside lactosylceramide (1 -30 pM), which lacks the Neu and galactosyl(P1-3)N-acetylgalactosamine moieties of the ganglioside, were found not to perturb (E)S3c fluorescence when mixed with the peptide (data not shown). The findings with lactosylceramide are similar to those of Saukkonen et al (1992), who found by TLC that this glycolipid was only recognised by the S2 subunit and not the S3 subunit of PT.…”

Section: (E)s3c Fluorescencesupporting

confidence: 88%

“…Previously, this technique has primarily been applied to the identification of peptides which represent subsites of anti-protein serum epitopes (Getzoff et al, 1987). The localised glycoprotein-binding region of S3 is closely analogous to the recently defined region I1 of a carbohydraterecognition domain proposed for the S3 subunit (Saukkonen et al, 1992). The possibility of multiple regions of S3 contributing to receptor binding cannot be excluded on the basis of our peptide-mapping results.…”

Section: Discussionsupporting

confidence: 71%

“…PT can function as one of the B. pertussis adhesins, which facilitate the first stage of infection by enabling attachment of the bacteria to the cilia of the respiratory tract (Relman et al, 1990;Saukkonen et al, 1992). In addition, several of the systemic disease effects which may result from infection, such as lymphocytosis, enhanced vascular permeability and stimulation of insulin secretion, can be reproduced by PT in experimental models (Ui, 1988).…”

Section: (Received November 2 1992) -Ejb 92 1550mentioning

confidence: 99%

“…The interaction of the B-oligomer with eukaryotic membrane glycoproteins and glycolipids is primarily mediated by subunits S2 and S3 (Capiau et d., 1986;Schmidt et al, 1991), which are both closely associated in the B-oligomer with subunit S4 (Tamura et al, 1982). S2 and S3 differ in their range of receptorbinding specificities, but also possess some receptors in common (Witvliet et al, 1989;Saukkonen et al, 1992). Attachment of the holotoxin to a target cell is considered to be followed by penetration of the target cell membrane by the catalytic S1 subunit (Ui, 1988).…”

Section: (Received November 2 1992) -Ejb 92 1550mentioning

confidence: 99%

“…Optimal binding of PT to glycoprotein depends upon the presence of N-acetylneuraminic acid and lactosamine constituents in the oligosaccharide (Armstrong et al, 1988;Witliviet et al, 1989). Furthermore, the existence of carbohydrate recognising domains in both the S2 and S3 subunits, has recently been c o n f i e d using site-directed mutants of PT (Saukkonen et al, 1992). Since certain carbohydrate-recognising domains of other proteins, such as fibronectin (Pierschbacher and Ruoslahti, 1984), have been mimicked by linear-peptide analogues, we have chosen to assess whether a peptide from the amino acid sequence of the S3 subunit of PT could also bind either glycoprotein or glycolipid.…”

Section: (Received November 2 1992) -Ejb 92 1550mentioning

confidence: 99%

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Localisation of a receptor‐recognition domain on the S3 subunit of pertussis toxin by peptide mapping

Tallett

Seabrook

Irons

et al. 1993

European Journal of Biochemistry

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Overlapping 1 O-amino-acid peptides, which consecutively span the amino acid sequence of the S3 subunit of pertussis toxin, were synthesised on polyethylene pins and screened for their ability to bind the glycoprotein fetuin. Fetuin binding was localised to a single peptide comprising amino acids 46-55. A free peptide, (E)S3c, of longer sequence (S3 amino acids 44-58) was also found to bind a-1 -acid glycoprotein, mixed brain gangliosides and fetuin. (E)S3c also recognised asialofetuin but with a lower apparent affinity relative to fetuin. The single tryptophan residue of the peptide yielded a fluorescence-emission maximum of 355 nm. In the presence of either ganglioside or the phospholipid L-a-lysolecithin, but not N-acetylneuramin-lactose or lactosylceramide, the emission intensity of (E)S3c was enhanced and the emission maximum blue-shifted to 340 nm by ganglioside, or to 345 nm by L-a-lysolecithin. Monosialogangliosides, disialogangliosides, and trisialogangliosides, when fluorescence-titrated, were each found to bind the peptide with a similar dissociation constant of 4.4 2 2.8 pM. These findings demonstrate that region 44-58 of the pertussis-toxin S3 subunit is likely to be involved in the recognition of both glycosylated and phospholipid constituents of target-cell membranes.

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Section: (E)s3c Fluorescencesupporting

confidence: 88%

Section: Discussionsupporting

confidence: 71%

Section: (Received November 2 1992) -Ejb 92 1550mentioning

confidence: 99%

Section: (Received November 2 1992) -Ejb 92 1550mentioning

confidence: 99%

Section: (Received November 2 1992) -Ejb 92 1550mentioning

confidence: 99%

See 3 more Smart Citations

Localisation of a receptor‐recognition domain on the S3 subunit of pertussis toxin by peptide mapping

Tallett

Seabrook

Irons

et al. 1993

European Journal of Biochemistry

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Bordetella pertussis toxin induces the release of inflammatory cytokines and dendritic cell activation in whole blood: impaired responses in human newborns

et al. 2002

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The regulatory roles of glycosphingolipid‐enriched lipid rafts in immune systems

et al. 2018

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Lipid rafts formed by glycosphingolipids (GSLs) on cellular membranes play important roles in innate and adaptive immunity. Lactosylceramide (LacCer) forms lipid rafts on plasma and granular membranes of human neutrophils. These LacCer‐enriched lipid rafts bind directly to pathogenic components, such as pathogenic fungi‐derived β‐glucan and Mycobacteria‐derived lipoarabinomannan via carbohydrate‐carbohydrate interactions, and mediate innate immune responses to these pathogens. In contrast, a‐series and o‐series gangliosides form distinct rafts on CD4+ and CD8+ T cell subsets, respectively, contributing to the respective functions of these cells and stimulating adaptive immune responses through T cell receptors. These findings suggest that gangliosides play indispensable roles in T cell selection and activation. This Review introduces the involvement of GSL‐enriched lipid rafts in innate and adaptive immunity.

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Pertussis toxin has eukaryotic-like carbohydrate recognition domains.

Cited by 125 publications

References 27 publications

Localisation of a receptor‐recognition domain on the S3 subunit of pertussis toxin by peptide mapping

Localisation of a receptor‐recognition domain on the S3 subunit of pertussis toxin by peptide mapping

Bordetella pertussis toxin induces the release of inflammatory cytokines and dendritic cell activation in whole blood: impaired responses in human newborns

The regulatory roles of glycosphingolipid‐enriched lipid rafts in immune systems

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