Interaction of two variable proteins (PilE and PilC) required for pilus‐mediated adherence of <i>Neisseria gonorrhoeae</i> to human epithelial cells

Rudel, Thomas; Putten, J. P. M. Van; Gibbs, Carol P.; Haas, Rainer; Meyer, Thomas F.

doi:10.1111/j.1365-2958.1992.tb02211.x

Cited by 198 publications

(225 citation statements)

References 47 publications

(6 reference statements)

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“…We found that four pili variants containing different PilE sequences (38) bound C4BP with similar apparent affinities (not shown). PilC is a 110-kDa pilus biogenesis protein that seems to be involved in the interaction between pili and MCP, because it was possible to select or genetically construct adherence negative mutants that expressed pili without detectable amounts of PilC (39,40). The results of an overlay assay suggested that C4BP interacts with the PilC subunit of pili.…”

Section: Discussionmentioning

confidence: 99%

A Novel Interaction Between Type IV Pili ofNeisseria gonorrhoeaeand the Human Complement Regulator C4b-Binding Protein

Blom

Rytkönen

Vásquez

et al. 2001

The Journal of Immunology

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C4b-binding protein (C4BP) is an important plasma inhibitor of the classical pathway of complement activation. Several bacterial pathogens bind C4BP, which may contribute to their virulence. In the present report we demonstrate that isolated type IV pili from Neisseria gonorrhoeae bind human C4BP in a dose-dependent and saturable manner. C4BP consists of seven identical α-chains and one β-chain linked together with disulfide bridges. We found that pili bind to the α-chain of C4BP, which is composed of eight homologous complement control protein (CCP) domains. From the results of an inhibition assay with C4b and a competition assay in which we tested mutants of C4BP lacking individual CCPs, we concluded that the binding area for pili is localized to CCP1 and CCP2 of the α-chain. The binding between pili and C4BP was abolished at 0.25 M NaCl, implying that it is based mostly on ionic interactions, similarly to what have been observed for C4b-C4BP binding. Furthermore, the N-terminal part of PilC, a structural component of pili, appeared to be responsible for binding of C4BP. Membrane cofactor protein, previously shown to be a receptor for pathogenic N. gonorrhoeae on the surface of epithelial cells, competed with C4BP for binding to pili only at high concentrations, suggesting that different parts of pili are involved in these two interactions. Accordingly, high concentrations of C4BP were required to inhibit binding of N. gonorrhoeae to Chang conjunctiva cells, and no inhibition of binding was observed with cervical epithelial cells.

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Section: Discussionmentioning

confidence: 99%

A Novel Interaction Between Type IV Pili ofNeisseria gonorrhoeaeand the Human Complement Regulator C4b-Binding Protein

Blom

Rytkönen

Vásquez

et al. 2001

The Journal of Immunology

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“…A 110-kD protein, pilC, present in small amounts in pill, is responsible for adherence to epithelial cells. The expression of this protein is subject to high frequency variation by a frame-shift mechanism due to a stretch of G residues early in the coding frame (10,11). The opacity proteins (opa) are also important adhesins.…”

Section: Discussionmentioning

confidence: 99%

“…This suggested that the high frequency antigenic variation of GC LOS could be due to slipped strand mispairing during replication, causing premature termination of translation. This form of variation has been seen in the case of the pilC protein (10), a G.C pilus accessory protein imparting adhesiveness to epithelial cells (11). The glycosyl transferases that might be subject to this form of variation are IgtA, the GlcNAc transfer~tse; lgtD, the GalNAc transferase; and IgtC, the Gal Xransferase responsible for the addition of o~Gall-4f3Gal.…”

Section: Sultlnlarymentioning

confidence: 99%

Variation of gonococcal lipooligosaccharide structure is due to alterations in poly-G tracts in lgt genes encoding glycosyl transferases.

Yang

Gotschlich

1996

The Journal of Experimental Medicine

116

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SUlTlnlaryThe lipooligosaccharide (LOS) expressed by gonococci spontaneously varies its structure at high frequency, but the underlying genetic mechanism has not been described. We have previously reported that the genes encoding the glycosyl transferases responsible for the biosynthesis of the variable o~ chain of the LOS of Neisseria gonorrhoeae are located in a locus containing five genes, lgtA, lgtB, IgtC, IgtD, and lgtE. Sequence analysis showed that tgtA, lgtC, and IgtD contained poly-G tracts within the coding frames, leading to the hypothesis that shiftsin the number of guanosine residues in the poly-G tracts might be responsible for the.high frequency variation in structure of gonococcal LOS. We now provide experimental evidence confirming this hypothesis.

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“…However, several studies have suggested a role for the pilin subunit PilE in receptor recognition. These include numerous findings showing that different antigenic variant forms of PilE influence epithelial cell adherence and tissue tropism (12,(14)(15)(16). However, the structural and functional attributes of PilE accounting for these observations remain unknown.…”

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confidence: 99%

“…The conclusion that PilC is a neisserial Tfp-associated adhesin is based primarily on the findings that (i) purified recombinant PilC imparts human epithelial cell binding activity on latex beads to which it has been coupled and blocks binding of piliated organisms to human epithelial cells (7) and (ii) piliated mutants lacking PilC fail to adhere (12,13). However, several studies have suggested a role for the pilin subunit PilE in receptor recognition.…”

mentioning

confidence: 99%

Neisseria gonorrhoeae PilV, a type IV pilus-associated protein essential to human epithelial cell adherence

Winther‐Larsen

Hegge

Wolfgang

et al. 2001

Proc. Natl. Acad. Sci. U.S.A.

121

136

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Type IV pili (Tfp) of Neisseria gonorrhoeae, the Gram-negative etiologic agent of gonorrhea, facilitate colonization of the human host. Tfp are assumed to play a key role in the initial adherence to human epithelial cells by virtue of the associated adhesin protein PilC. To examine the structural and functional basis for adherence in more detail, we identified potential genes encoding polypeptides sharing structural similarities to PilE (the Tfp subunit) within the N. gonorrhoeae genome sequence database. We show here that a fiber subunit-like protein, termed PilV, is essential to organelle-associated adherence but dispensable for Tfp biogenesis and other pilus-related phenotypes, including autoagglutination, competence for natural transformation, and twitching motility. The adherence defect in pilV mutants cannot be attributed to reduced levels of piliation, defects in fiber anchoring to the bacterial cell surface, or to unstable pilus expression related to organelle retraction. PilV is expressed at low levels relative to PilE and copurifies with Tfp fibers in a PilC-dependent fashion. Purified Tfp from pilV mutants contain PilC adhesin at reduced levels. Taken together, these data support a model in which PilV functions in adherence by promoting the functional display of PilC in the context of the pilus fiber.

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Interaction of two variable proteins (PilE and PilC) required for pilus‐mediated adherence of Neisseria gonorrhoeae to human epithelial cells

Cited by 198 publications

References 47 publications

A Novel Interaction Between Type IV Pili ofNeisseria gonorrhoeaeand the Human Complement Regulator C4b-Binding Protein

A Novel Interaction Between Type IV Pili ofNeisseria gonorrhoeaeand the Human Complement Regulator C4b-Binding Protein

Variation of gonococcal lipooligosaccharide structure is due to alterations in poly-G tracts in lgt genes encoding glycosyl transferases.

Neisseria gonorrhoeae PilV, a type IV pilus-associated protein essential to human epithelial cell adherence

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