Identification of two protein-binding and functional regions of curli, a surface organelle and virulence determinant of Escherichia coli

Olsén, Arne; Herwald, Heiko; Wikstrom, M; Persson, Kristin; Mattsson, Eva; Björck, Lars

Identification of two protein-binding and functional regions of curli, a surface organelle and virulence determinant of Escherichia coli

Mark

; Wikstrom, M ; Persson, Kristin ^LU ; Mattsson, Eva ^LU and Björck, Lars ^LU (2002) In Journal of Biological Chemistry 277(37). p.34568-34572

Abstract: Curli are surface organelles of Escherichia coli. These fibrous proteins, formed by polymerization of a 15-kDa subunit, are expressed by E. coli strains associated with severe infections in humans. A remarkable property of curli is their ability to interact with a wide range of human proteins, interactions that contribute to the enhanced virulence of curli-expressing E. coli. To define the protein-binding region(s) of curli, we investigated the binding properties of overlapping synthetic peptides covering the curli subunit. Two peptides, one covering a 24-amino acid residue sequence in the NH2-terminal half of the subunit (NNS24) and one corresponding to the 26 COOH-terminal residues (VDQ26), were found to bind a number of human proteins.... (More); Curli are surface organelles of Escherichia coli. These fibrous proteins, formed by polymerization of a 15-kDa subunit, are expressed by E. coli strains associated with severe infections in humans. A remarkable property of curli is their ability to interact with a wide range of human proteins, interactions that contribute to the enhanced virulence of curli-expressing E. coli. To define the protein-binding region(s) of curli, we investigated the binding properties of overlapping synthetic peptides covering the curli subunit. Two peptides, one covering a 24-amino acid residue sequence in the NH2-terminal half of the subunit (NNS24) and one corresponding to the 26 COOH-terminal residues (VDQ26), were found to bind a number of human proteins. Physiochemical analysis revealed that NNS24 adopts a thermally stable beta-structure, and in solution the peptide forms soluble multimers, predominantly octamers. Intact curli are known to activate the proinflammatory and procoagulant contact system, and when added to human plasma, the NNS24 and VDQ26 peptides induced the release of the potent vasoactive peptide bradykinin. The results map important curli functions to the regions corresponding to the NNS24 and VDQ26 sequences. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/328576

author

Olsén, Arne ^LU ; Herwald, Heiko ^LU

; Wikstrom, M ; Persson, Kristin ^LU ; Mattsson, Eva ^LU and Björck, Lars ^LU

organization

publishing date

2002

type

Contribution to journal

publication status

published

subject

Infectious Medicine

in

Journal of Biological Chemistry

volume

277

issue

37

pages

34568 - 34572

publisher

American Society for Biochemistry and Molecular Biology

external identifiers

wos:000177959100130
scopus:0037072888

ISSN

1083-351X

DOI

10.1074/jbc.M206353200

language

English

LU publication?

yes

id

60eb2c75-a128-4fab-9889-46f31fd0a0e1 (old id 328576)

date added to LUP

2016-04-01 12:38:02

date last changed

2022-01-27 07:44:57

@article{60eb2c75-a128-4fab-9889-46f31fd0a0e1,
  abstract     = {{Curli are surface organelles of Escherichia coli. These fibrous proteins, formed by polymerization of a 15-kDa subunit, are expressed by E. coli strains associated with severe infections in humans. A remarkable property of curli is their ability to interact with a wide range of human proteins, interactions that contribute to the enhanced virulence of curli-expressing E. coli. To define the protein-binding region(s) of curli, we investigated the binding properties of overlapping synthetic peptides covering the curli subunit. Two peptides, one covering a 24-amino acid residue sequence in the NH2-terminal half of the subunit (NNS24) and one corresponding to the 26 COOH-terminal residues (VDQ26), were found to bind a number of human proteins. Physiochemical analysis revealed that NNS24 adopts a thermally stable beta-structure, and in solution the peptide forms soluble multimers, predominantly octamers. Intact curli are known to activate the proinflammatory and procoagulant contact system, and when added to human plasma, the NNS24 and VDQ26 peptides induced the release of the potent vasoactive peptide bradykinin. The results map important curli functions to the regions corresponding to the NNS24 and VDQ26 sequences.}},
  author       = {{Olsén, Arne and Herwald, Heiko and Wikstrom, M and Persson, Kristin and Mattsson, Eva and Björck, Lars}},
  issn         = {{1083-351X}},
  language     = {{eng}},
  number       = {{37}},
  pages        = {{34568--34572}},
  publisher    = {{American Society for Biochemistry and Molecular Biology}},
  series       = {{Journal of Biological Chemistry}},
  title        = {{Identification of two protein-binding and functional regions of curli, a surface organelle and virulence determinant of Escherichia coli}},
  url          = {{http://dx.doi.org/10.1074/jbc.M206353200}},
  doi          = {{10.1074/jbc.M206353200}},
  volume       = {{277}},
  year         = {{2002}},
}

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Identification of two protein-binding and functional regions of curli, a surface organelle and virulence determinant of Escherichia coli