AmiA is a penicillin target enzyme with dual activity in the intracellular pathogen Chlamydia pneumoniae

[en] Intracellular Chlamydiaceae do not need to resist osmotic challenges and a functional cell wall was not detected in these pathogens. Nevertheless, a recent study revealed evidence for circular peptidoglycan-like structures in Chlamydiaceae and penicillin inhibits cytokinesis, a phenomenon known as the chlamydial anomaly. Here, by characterizing a cell wall precursor-processing enzyme, we provide insights into the mechanisms underlying this mystery. We show that AmiA from Chlamydia pneumoniae separates daughter cells in an Escherichia coli amidase mutant. Contrary to homologues from free-living bacteria, chlamydial AmiA uses lipid II as a substrate and has dual activity, acting as an amidase and a carboxypeptidase. The latter function is penicillin sensitive and assigned to a penicillin-binding protein motif. Consistent with the lack of a regulatory domain in AmiA, chlamydial CPn0902, annotated as NlpD, is a carboxypeptidase, rather than an amidase activator, which is the case for E. coli NlpD. Functional conservation of AmiA implicates a role in cytokinesis and host response modulation.

Disciplines :

Biochemistry, biophysics & molecular biology

Author, co-author :

Klockner, Anna

Otten, Christian

Derouaux, Adeline ; Université de Liège - ULiège > GIGA-R : Virologie - Immunologie

Vollmer, Waldemar

Buhl, Henrike

De Benedetti, Stephania

Munch, Daniela

Josten, Michaele

Molleken, Katja

Sahl, Hans-Georg

Henrichfreise, Beate

Language :

English

Title :

AmiA is a penicillin target enzyme with dual activity in the intracellular pathogen Chlamydia pneumoniae

Publication date :

2014

Journal title :

Nature Communications

eISSN :

2041-1723

Publisher :

Nature Pub.lishing Group, London, United Kingdom

Peer reviewed :

Peer Reviewed verified by ORBi

Available on ORBi :

since 05 January 2015

Statistics

Number of views

54 (0 by ULiège)

Number of downloads

1 (0 by ULiège)

More statistics

Scopus citations^®

Scopus citations^®
without self-citations

OpenCitations

OpenAlex citations

See more details

publications

supporting

mentioning

contrasting

Smart Citations

Citing PublicationsSupportingMentioningContrasting

View Citations

See how this article has been cited at scite.ai

scite shows how a scientific paper has been cited by providing the context of the citation, a classification describing whether it supports, mentions, or contrasts the cited claim, and a label indicating in which section the citation was made.

Bibliography

McCoy, A.J., Maurelli, A.T., Building the invisible wall: Updating the chlamydial peptidoglycan anomaly (2006) Trends in Microbiology, 14 (2), pp. 70-77. , DOI 10.1016/j.tim.2005.12.004, PII S0966842X05003355
Hafner, L.M., Timms, P., Persistent chlamydial infections: Role in inflammation and challenges for vaccine development (2005) Mucosal Immunol. Update, 13, pp. 4-7
Typas, A., Banzhaf, M., Gross, C.A., Vollmer, W., From the regulation of peptidoglycan synthesis to bacterial growth and morphology (2012) Nat. Rev. Microbiol., 10, pp. 123-136
Lutkenhaus, J., Pichoff, S., Du, S., Bacterial cytokinesis: From Z ring to divisome (2012) Cytoskeleton (Hoboken), 69, pp. 778-790
Pinho, M.G., Kjos, M., Veening, J.W., How to get (a)round: Mechanisms controlling growth and division of coccoid bacteria (2013) Nat. Rev. Microbiol., 11, pp. 601-614
Heidrich, C., Templin, M.F., Ursinus, A., Merdanovic, M., Berger, J., Schwarz, H., De Pedro, M.A., Holtje, J.-V., Involvement of N-acetylmuramyl-L-alanine amidases in cell separation and antibiotic-induced autolysis of Escherichia coli (2001) Molecular Microbiology, 41 (1), pp. 167-178. , DOI 10.1046/j.1365-2958.2001.02499.x
Priyadarshini, R., De Pedro, M.A., Young, K.D., Role of peptidoglycan amidases in the development and morphology of the division septum in Escherichia coli (2007) Journal of Bacteriology, 189 (14), pp. 5334-5347. , DOI 10.1128/JB.00415-07
Uehara, T., Parzych, K.R., Dinh, T., Bernhardt, T.G., Daughter cell separation is controlled by cytokinetic ring-activated cell wall hydrolysis (2010) EMBO J., 29, pp. 1412-1422
Lupoli, T.J., Studying a cell division amidase using defined peptidoglycan substrates (2009) J. Am. Chem. Soc., 131, pp. 18230-18231
McCoy, A.J., Adams, N.E., Hudson, A.O., Gilvarg, C., Leustek, T., Maurelli, A.T., L,L-diaminopimelate aminotransferase, a trans-kingdom enzyme shared by Chlamydia and plants for synthesis of diaminopimelate/lysine (2006) Proceedings of the National Academy of Sciences of the United States of America, 103 (47), pp. 17909-17914. , DOI 10.1073/pnas.0608643103
Patin, D., Bostock, J., Blanot, D., Mengin-Lecreulx, D., Chopra, I., Functional and biochemical analysis of the Chlamydia trachomatis ligase MurE (2009) J. Bacteriol., 191, pp. 7430-7435
De Benedetti, S., Characterization of serine hydroxymethyltransferase GlyA as a potential source of D-alanine in Chlamydia pneumoniae (2014) Front. Cell. Infect. Microbiol., 4, p. 19
Henrichfreise, B., Functional conservation of the lipid II biosynthesis pathway in the cell wall-less bacteria Chlamydia and Wolbachia: Why is lipid II needed? (2009) Mol. Microbiol., 73, pp. 913-923
Patin, D., Bostock, J., Chopra, I., Mengin-Lecreulx, D., Blanot, D., Biochemical characterisation of the chlamydial MurF ligase, and possible sequence of the chlamydial peptidoglycan pentapeptide stem (2012) Arch. Microbiol., 194, pp. 505-512
Gaballah, A., Kloeckner, A., Otten, C., Sahl, H.G., Henrichfreise, B., Functional analysis of the cytoskeleton protein MreB from Chlamydophila pneumoniae (2011) PLoS ONE, 6, pp. e25129
Pilhofer, M., Discovery of chlamydial peptidoglycan reveals bacteria with murein sacculi but without FtsZ (2013) Nat. Commun., 4, p. 2856
Jacquier, N., Frandi, A., Pillonel, T., Viollier, P., Greub, G., Cell wall precursors are required to organize the chlamydial division septum (2014) Nat. Commun., 5, p. 3578
Liechti, G.W., A new metabolic cell-wall labelling method reveals peptidoglycan in Chlamydia trachomatis (2014) Nature, 506, pp. 507-510
Joris, B., The active-site-serine penicillin-recognizing enzymes as members of the Streptomyces R61 DD-peptidase family (1988) Biochem. J., 250, pp. 313-324
Ghosh, A.S., Chowdhury, C., Nelson, D.E., Physiological functions of D-alanine carboxypeptidases in Escherichia coli (2008) Trends Microbiol., 16, pp. 309-317
Arthur, M., Depardieu, F., Cabanie, L., Reynolds, P., Courvalin, P., Requirement of the VanY and VanX D,D-peptidases for glycopeptide resistance in enterococci (1998) Molecular Microbiology, 30 (4), pp. 819-830. , DOI 10.1046/j.1365-2958.1998.01114.x
Wright, G.D., Molinas, C., Arthur, M., Courvalin, P., Walsh, C.T., Characterization of vanY, a DD-carboxypeptidase from vancomycin-resistant Enterococcus faecium BM4147 (1992) Antimicrob. Agents. Chemother., 36, pp. 1514-1518
Hooper, N.M., Families of zinc metalloproteases (1994) FEBS Letters, 354 (1), pp. 1-6. , DOI 10.1016/0014-5793(94)01079-X
Reynolds, P.E., Ambur, O.H., Casadewall, B., Courvalin, P., The VanYD DD-carboxypeptidase of Enterococcus faecium BM4339 is a penicillin-binding protein (2001) Microbiology, 147 (9), pp. 2571-2578
Yang, D.C., Tan, K., Joachimiak, A., Bernhardt, T.G., A conformational switch controls cell wall-remodelling enzymes required for bacterial cell division (2012) Mol. Microbiol., 85, pp. 768-781
Holm, L., Rosenström, P., Dali server: Conservation mapping in 3D (2010) Nucleic Acids Res., 38, pp. W545-W549
Hourdou, M.L., Characterization of the sporulation-related gamma-D-glutamyl-(L)meso- diaminopimelic-acid-hydrolysing peptidase i of Bacillus sphaericus NCTC 9602 as a member of the metallo(zinc) carboxypeptidase A family. Modular design of the protein (1993) Biochem. J., 292 (PART 2), pp. 563-570
Goffin, C., Ghuysen, J.-M., Biochemistry and comparative genomics of SxxK superfamily acyltransferases offer a clue to the mycobacterial paradox: Presence of penicillin-susceptible target proteins versus lack of efficiency of penicillin as therapeutic agent (2002) Microbiology and Molecular Biology Reviews, 66 (4), pp. 702-738. , DOI 10.1128/MMBR.66.4.702-738.2002
Vollmer, W., Blanot, D., De Pedro, M.A., Peptidoglycan structure and architecture (2008) FEMS Microbiology Reviews, 32 (2), pp. 149-167. , DOI 10.1111/j.1574-6976.2007.00094.x
Dilks, K., Rose, R.W., Hartmann, E., Pohlschroder, M., Prokaryotic utilization of the twin-arginine translocation pathway: A genomic survey (2003) Journal of Bacteriology, 185 (4), pp. 1478-1483. , DOI 10.1128/JB.185.4.1478-1483.2003
Bendtsen, J.D., Nielsen, H., Widdick, D., Palmer, T., Brunak, S., Prediction of twin-arginine signal peptides (2005) BMC Bioinformatics, 6, p. 167
Petersen, T.N., Brunak, S., Von Heijne, G., Nielsen, H., SignalP 4.0: Discriminating signal peptides from transmembrane regions (2011) Nat. Methods, 8, pp. 785-786
Yang, D.C., An ATP-binding cassette transporter-like complex governs cell-wall hydrolysis at the bacterial cytokinetic ring (2011) Proc. Natl Acad. Sci. USA, 108, pp. E1052-E1060
Frandi, FtsZ-independent septal recruitment and function of cell wall remodelling enzymes in chlamydial pathogens Nat. Commun., 5, p. 4200
Skilton, R.J., Penicillin induced persistence in Chlamydia trachomatis: High quality time lapse video analysis of the developmental cycle (2009) PLoS ONE, 4, pp. e7723
Tomasz, A., The mechanism of the irreversible antimicrobial effects of penicillins: How the beta-lactam antibiotics kill and lyse bacteria (1979) Annu. Rev. Microbiol., 33, pp. 113-137
Ghuysen, J.-M., Goffin, C., Lack of cell wall peptidoglycan versus penicillin sensitivity: New insights into the chlamydial anomaly (1999) Antimicrobial Agents and Chemotherapy, 43 (10), pp. 2339-2344
Tatar, L.D., Marolda, C.L., Polischuk, A.N., Van Leeuwen, D., Valvano, M.A., An Escherichia coli undecaprenyl-pyrophosphate phosphatase implicated in undecaprenyl phosphate recycling (2007) Microbiology, 153 (8), pp. 2518-2529. , DOI 10.1099/mic.0.2007/006312-0
Morlot, C., Uehara, T., Marquis, K.A., Bernhardt, T.G., Rudner, D.Z., A highly coordinated cell wall degradation machine governs spore morphogenesis in Bacillus subtilis (2010) Genes Dev., 24, pp. 411-422
Bourgeois, I., Characterization of AtlL, a bifunctional autolysin of Staphylococcus lugdunensis with N-acetylglucosaminidase and N-acetylmuramoyl-l-alanine amidase activities (2009) FEMS Microbiol. Lett., 290, pp. 105-113
Oshida, T., A Staphylococcus aureus autolysin that has an N-acetylmuramoyl-L-alanine amidase domain and an endo-beta-N-acetylglucosaminidase domain: Cloning, sequence analysis, and characterization (1995) Proc. Natl Acad. Sci. USA, 92, pp. 285-289
Ouellette, S.P., Karimova, G., Subtil, A., Ladant, D., Chlamydia co-opts the rod shape-determining proteins MreB and Pbp2 for cell division (2012) Mol. Microbiol., 85, pp. 164-178
Humann, J., Lenz, L.L., Bacterial peptidoglycan degrading enzymes and their impact on host muropeptide detection (2009) J. Innate Immun., 1, pp. 88-97
Girardin, S.E., Travassos, L.H., Herve, M., Blanot, D., Boneca, I.G., Philpott, D.J., Sansonetti, P.J., Mengin-Lecreulx, D., Peptidoglycan molecular requirements allowing detection by nod1 and nod2 (2003) Journal of Biological Chemistry, 278 (43), pp. 41702-41708. , DOI 10.1074/jbc.M307198200
Baba, T., Construction of Escherichia coli K-12 in-frame, single-gene knockout mutants: The Keio collection (2006) Mol. Syst. Biol., 2, p. 0008
Juhasz, P., Costello, C.E., Matrix-assisted laser desorption ionization time-offlight mass spectrometry of underivatized and permethylated gangliosides (1992) J. Am. Soc. Mass. Spectrom., 3, pp. 785-796
Hunter, S., InterPro in 2011: New developments in the family and domain prediction database (2012) Nucleic Acids Res., 40, pp. D306-D312
Krogh, A., Larsson, B., Von Heijne, G., Sonnhammer, E.L.L., Predicting transmembrane protein topology with a hidden Markov model: Application to complete genomes (2001) Journal of Molecular Biology, 305 (3), pp. 567-580. , DOI 10.1006/jmbi.2000.4315

Similar publications

Sorry the service is unavailable at the moment. Please try again later.