TY - JOUR
T1 - Rationally designed small compounds inhibit pilus biogenesis in uropathogenic bacteria
AU - Pinkner, Jerome S.
AU - Remaut, Han
AU - Buelens, Floris
AU - Miller, Eric
AU - Åberg, Veronica
AU - Pemberton, Nils
AU - Hedenström, Mattias
AU - Larsson, Andreas
AU - Seed, Patrick
AU - Waksman, Gabriel
AU - Hultgren, Scott J.
AU - Almqvist, Fredrik
PY - 2006/11/21
Y1 - 2006/11/21
N2 - A chemical synthesis platform with broad applications and flexibility was rationally designed to inhibit biogenesis of adhesive pili assembled by the chaperone-usher pathway in Gram-negative pathogens. The activity of a family of bicyclic 2-pyridones, termed pilicides, was evaluated in two different pilus biogenesis systems in uropathogenic Escherichia coli. Hemagglutination mediated by either type 1 or P pili, adherence to bladder cells, and biofilm formation mediated by type 1 pili were all reduced by ≈90% in laboratory and clinical E. coli strains. The structure of the pilicide bound to the P pilus chaperone PapD revealed that the pilicide bound to the surface of the chaperone known to interact with the usher, the outer-membrane assembly platform where pili are assembled. Point mutations in the pilicide-binding site dramatically reduced pilus formation but did not block the ability of PapD to bind subunits and mediate their folding. Surface plasmon resonance experiments confirmed that the pilicide interfered with the binding of chaperone-subunit complexes to the usher. These pilicides thus target key virulence factors in pathogenic bacteria and represent a promising proof of concept for developing drugs that function by targeting virulence factors.
AB - A chemical synthesis platform with broad applications and flexibility was rationally designed to inhibit biogenesis of adhesive pili assembled by the chaperone-usher pathway in Gram-negative pathogens. The activity of a family of bicyclic 2-pyridones, termed pilicides, was evaluated in two different pilus biogenesis systems in uropathogenic Escherichia coli. Hemagglutination mediated by either type 1 or P pili, adherence to bladder cells, and biofilm formation mediated by type 1 pili were all reduced by ≈90% in laboratory and clinical E. coli strains. The structure of the pilicide bound to the P pilus chaperone PapD revealed that the pilicide bound to the surface of the chaperone known to interact with the usher, the outer-membrane assembly platform where pili are assembled. Point mutations in the pilicide-binding site dramatically reduced pilus formation but did not block the ability of PapD to bind subunits and mediate their folding. Surface plasmon resonance experiments confirmed that the pilicide interfered with the binding of chaperone-subunit complexes to the usher. These pilicides thus target key virulence factors in pathogenic bacteria and represent a promising proof of concept for developing drugs that function by targeting virulence factors.
KW - Antimicrobials
KW - Chaperone-usher pathway
KW - Pilicide
KW - Urinary tract infection
UR - http://www.scopus.com/inward/record.url?scp=33845228423&partnerID=8YFLogxK
U2 - 10.1073/pnas.0606795103
DO - 10.1073/pnas.0606795103
M3 - Article
C2 - 17098869
AN - SCOPUS:33845228423
SN - 0027-8424
VL - 103
SP - 17897
EP - 17902
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 47
ER -