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Infect Immun, February 1998, p. 486-491, Vol. 66, No. 2
Laboratoire de Chimie Biologique, Unité
Mixte de Recherche du CNRS no. 111, Université des Sciences et
Technologies de Lille, 59655 Villeneuve d'Ascq Cedex,
France1;
Institut de Biochimie de
l'Académie Roumaine, Splaiul Independentei 296, 77.700 Bucharest 17, Rumania2; and
Department
of Immunology, Scripps Research Institute, La Jolla, California
920373
Received 24 July 1997/Returned for modification 24 September
1997/Accepted 11 November 1997
Human lactoferrin (hLf), a glycoprotein released from neutrophil
granules during inflammation, and the lipopolysaccharide (LPS)-binding
protein (LBP), an acute-phase serum protein, are known to bind to the
lipid A of LPS. The LPS-binding sites are located in the N-terminal
regions of both proteins, at amino acid residues 28 to 34 of hLf and 91 to 108 of LBP. Both of these proteins modulate endotoxin activities,
but they possess biologically antagonistic properties. In this study,
we have investigated the competition between hLf and recombinant human
LBP (rhLBP) for the binding of Escherichia coli 055:B5 LPS
to the differentiated monocytic THP-1 cell line. Our studies revealed
that hLf prevented the rhLBP-mediated binding of LPS to the CD14
receptor on cells. Maximal inhibition of LPS-cell interactions by hLf
was raised when both hLf and rhLBP were simultaneously added to LPS or
when hLf and LPS were mixed with cells 30 min prior to the incubation
with rhLBP. However, when hLf was added 30 min after the interaction of
rhLBP with LPS, the binding of the rhLPS-LBP complex to CD14 could not
be reversed. These observations indicate that hLf competes with rhLBP for the LPS binding and therefore interferes with the interaction of
LPS with CD14. Furthermore, experiments involving competitive binding
of the rhLBP-LPS complex to cells with two recombinant mutated hLfs
show that in addition to residues 28 to 34, another basic cluster which
contains residues 1 to 5 of hLf competes for the binding to LPS. Basic
sequences homologous to residues 28 to 34 of hLf were evidenced on
LPS-binding proteins such as LBP, bactericidal/permeability-increasing
protein, and Limulus anti-LPS factor.
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
Lactoferrin Inhibits the Endotoxin Interaction with
CD14 by Competition with the Lipopolysaccharide-Binding
Protein
*
Corresponding author. Mailing address: Laboratoire de
Chimie Biologique, Unité Mixte de Recherche du CNRS no. 111, Université des Sciences et Technologies de Lille, 59655 Villeneuve d'Ascq Cedex, France. Phone: 33.3.20.43.41.55. Fax:
33.3.20.43.65.55. E-mail: Genevieve.Spik{at}univ-lille1.fr.
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