2pzm Citations

Predicting protein function from structure--the roles of short-chain dehydrogenase/reductase enzymes in Bordetella O-antigen biosynthesis.

King JD, Harmer NJ, Preston A, Palmer CM, Rejzek M, Field RA, Blundell TL, Maskell DJ
J Mol Biol 374 749-63 (2007)
Related entries: 2pzj, 2pzk, 2pzl, 2q1s, 2q1t, 2q1u, 2q1w

Cited: 17 times
EuropePMC logo PMID: 17950751

Abstract

The pathogenic bacteria Bordetella parapertussis and Bordetella bronchiseptica express a lipopolysaccharide O antigen containing a polymer of 2,3-diacetamido-2,3-dideoxy-l-galacturonic acid. The O-antigen cluster contains three neighbouring genes that encode proteins belonging to the short-chain dehydrogenase/reductase (SDR) family, wbmF, wbmG and wbmH, and we aimed to elucidate their individual functions. Mutation and complementation implicate each gene in O-antigen expression but, as their putative sugar nucleotide substrates are not currently available, biochemical characterisation of WbmF, WbmG and WbmH is impractical at the present time. SDR family members catalyse a wide range of chemical reactions including oxidation, reduction and epimerisation. Because they typically share low sequence conservation, however, catalytic function cannot be predicted from sequence analysis alone. In this context, structural characterisation of the native proteins, co-crystals and small-molecule soaks enables differentiation of the functions of WbmF, WbmG and WbmH. These proteins exhibit typical SDR architecture and coordinate NAD. In the substrate-binding domain, all three enzymes bind uridyl nucleotides. WbmG contains a typical SDR catalytic TYK triad, which is required for oxidoreductase function, but the active site is devoid of additional acid-base functionality. Similarly, WbmH possesses a TYK triad, but an otherwise feature-poor active site. Consequently, 3,5-epimerase function can probably be ruled out for these enzymes. The WbmF active site contains conserved 3,5-epimerase features, namely, a positionally conserved cysteine (Cys133) and basic side chain (His90 or Asn213), but lacks the serine/threonine component of the SDR triad and therefore may not act as an oxidoreductase. The data suggest a pathway for synthesis of the O-antigen precursor UDP-2,3-diacetamido-2,3-dideoxy-l-galacturonic acid and illustrate the usefulness of structural data in predicting protein function.

Articles - 2pzm mentioned but not cited (2)

  1. Predicting protein function from structure--the roles of short-chain dehydrogenase/reductase enzymes in Bordetella O-antigen biosynthesis. King JD, Harmer NJ, Preston A, Palmer CM, Rejzek M, Field RA, Blundell TL, Maskell DJ. J Mol Biol 374 749-763 (2007)
  2. Cloning, expression, purification and preliminary crystallographic analysis of the short-chain dehydrogenase enzymes WbmF, WbmG and WbmH from Bordetella bronchiseptica. Harmer NJ, King JD, Palmer CM, Preston A, Maskell DJ, Blundell TL. Acta Crystallogr Sect F Struct Biol Cryst Commun 63 711-715 (2007)


Reviews citing this publication (2)

  1. Review: Lipopolysaccharide biosynthesis in Pseudomonas aeruginosa. King JD, Kocíncová D, Westman EL, Lam JS. Innate Immun 15 261-312 (2009)
  2. A survey of chemical methods for sugar-nucleotide synthesis. Wagner GK, Pesnot T, Field RA. Nat Prod Rep 26 1172-1194 (2009)

Articles citing this publication (13)

  1. Architecture of mammalian respiratory complex I. Vinothkumar KR, Zhu J, Hirst J. Nature 515 80-84 (2014)
  2. The structural basis for catalytic function of GMD and RMD, two closely related enzymes from the GDP-D-rhamnose biosynthesis pathway. King JD, Poon KKH, Webb NA, Anderson EM, McNally DJ, Brisson JR, Messner P, Garavito RM, Lam JS. FEBS J 276 2686-2700 (2009)
  3. Biosynthesis of a rare di-N-acetylated sugar in the lipopolysaccharides of both Pseudomonas aeruginosa and Bordetella pertussis occurs via an identical scheme despite different gene clusters. Westman EL, Preston A, Field RA, Lam JS. J Bacteriol 190 6060-6069 (2008)
  4. Comparison of predicted epimerases and reductases of the Campylobacter jejuni D-altro- and L-gluco-heptose synthesis pathways. McCallum M, Shaw GS, Creuzenet C. J Biol Chem 288 19569-19580 (2013)
  5. Characterization of WbpB, WbpE, and WbpD and reconstitution of a pathway for the biosynthesis of UDP-2,3-diacetamido-2,3-dideoxy-D-mannuronic acid in Pseudomonas aeruginosa. Westman EL, McNally DJ, Charchoglyan A, Brewer D, Field RA, Lam JS. J Biol Chem 284 11854-11862 (2009)
  6. Biosynthesis of uronamide sugars in Pseudomonas aeruginosa O6 and Escherichia coli O121 O antigens. King JD, Vinogradov E, Tran V, Lam JS. Environ Microbiol 12 1531-1544 (2010)
  7. Approaching boiling point stability of an alcohol dehydrogenase through computationally-guided enzyme engineering. Aalbers FS, Fürst MJ, Rovida S, Trajkovic M, Gómez Castellanos JR, Bartsch S, Vogel A, Mattevi A, Fraaije MW. Elife 9 e54639 (2020)
  8. Antigenic Variation among Bordetella: Bordetella bronchiseptica strain MO149 expresses a novel o chain that is poorly immunogenic. Vinogradov E, King JD, Pathak AK, Harvill ET, Preston A. J Biol Chem 285 26869-26877 (2010)
  9. Chemical synthesis of UDP-Glc-2,3-diNAcA, a key intermediate in cell surface polysaccharide biosynthesis in the human respiratory pathogens B. pertussis and P. aeruginosa. Rejzek M, Sri Kannathasan V, Wing C, Preston A, Westman EL, Lam JS, Naismith JH, Maskell DJ, Field RA. Org Biomol Chem 7 1203-1210 (2009)
  10. Engineering an Alcohol-Forming Fatty Acyl-CoA Reductase for Aldehyde and Hydrocarbon Biosynthesis in Saccharomyces cerevisiae. Foo JL, Rasouliha BH, Susanto AV, Leong SSJ, Chang MW. Front Bioeng Biotechnol 8 585935 (2020)
  11. Biosynthetic access to the rare antiarose sugar via an unusual reductase-epimerase. Yan Y, Yang J, Wang L, Xu D, Yu Z, Guo X, Horsman GP, Lin S, Tao M, Huang SX. Chem Sci 11 3959-3964 (2020)
  12. Developing an asymmetric, stereodivergent route to selected 6-deoxy-6-fluoro-hexoses. Caravano A, Field RA, Percy JM, Rinaudo G, Roig R, Singh K. Org Biomol Chem 7 996-1008 (2009)
  13. AMP-dependent phosphite dehydrogenase, a phosphorylating enzyme in dissimilatory phosphite oxidation. Mao Z, Fleming JR, Mayans O, Frey J, Schleheck D, Schink B, Müller N. Proc Natl Acad Sci U S A 120 e2309743120 (2023)


Related citations provided by authors (1)

  1. Cloning, expression, purification and preliminary crystallographic analysis of the short-chain dehydrogenase enzymes WbmF, WbmG and WbmH from Bordetella bronchiseptica.. Harmer NJ, King JD, Palmer CM, Preston A, Maskell DJ, Blundell TL Acta Crystallogr Sect F Struct Biol Cryst Commun 63 711-5 (2007)

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