Crystal Structure of 4-Oxalocrotonate Tautomerase Inactivated by 2-Oxo-3-pentynoate at 2.4 Å Resolution:  Analysis and Implications for the Mechanism of Inactivation and Catalysis<sup>,</sup>

Taylor, Alexander B.; Czerwiński, Robert; Johnson, William H.; Whitman, Christian P.; Hackert, Marvin L.

doi:10.1021/bi981607j

Cited by 73 publications

(170 citation statements)

References 29 publications

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“…In contrast to the presence of potentially six active sites in the highly symmetrical 4-OT molecule (45), there are three potential active sites in CaaD. From the crystal structure of 4-OT inactivated by 2-oxo-3-pentynoate (45), the substrate should interact with Pro-1 of one subunit and Arg-11 from an adjacent subunit within the same homodimer.…”

Section: Discussionmentioning

confidence: 99%

trans -3-Chloroacrylic Acid Dehalogenase from Pseudomonas pavonaceae 170 Shares Structural and Mechanistic Similarities with 4-Oxalocrotonate Tautomerase

2001

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The genes (caaD1 and caaD2) encoding the trans-3-chloroacrylic acid dehalogenase (CaaD) of the 1,3-dichloropropene-utilizing bacterium Pseudomonas pavonaceae 170 were cloned and heterologously expressed in Escherichia coli and Pseudomonas sp. strain GJ1. CaaD is a protein of 50 kDa that is composed of ␣-subunits of 75 amino acid residues and ␤-subunits of 70 residues. It catalyzes the hydrolytic cleavage of the ␤-vinylic carbonchlorine bond in trans-3-chloroacrylic acid with a turnover number of 6.4 s ؊1. On the basis of sequence similarity, oligomeric structure, and subunit size, CaaD appears to be related to 4-oxalocrotonate tautomerase (4-OT). This tautomerase consists of six identical subunits of 62 amino acid residues and catalyzes the isomerization of 2-oxo-4-hexene-1,6-dioate, via hydroxymuconate, to yield 2-oxo-3-hexene-1,6-dioate. In view of the oligomeric architecture of 4-OT, a trimer of homodimers, CaaD is postulated to be a hexameric protein that functions as a trimer of ␣␤-dimers. The sequence conservation between CaaD and 4-OT and site-directed mutagenesis experiments suggested that Pro-1 of the ␤-subunit and Arg-11 of the ␣-subunit are active-site residues in CaaD. Pro-1 could act as the proton acceptor/donor, and Arg-11 is probably involved in carboxylate binding. Based on these findings, a novel dehalogenation mechanism is proposed for the CaaD-catalyzed reaction which does not involve the formation of a covalent enzyme-substrate intermediate.Isomer-specific 3-chloroacrylic acid dehalogenases catalyze the hydrolytic cleavage of the ␤-vinylic carbon-chlorine bond in either cis-or trans-3-chloroacrylic acid to yield malonic acid semialdehyde and HCl. These enzymes are produced by both gram-positive and gram-negative bacteria, including Pseudomonas pavonaceae 170 (27), Pseudomonas cepacia CAA1 (11), and the coryneform bacterial strains FG41 (47) and CAA2 (11), enabling these organisms to use one or both isomers of the xenobiotic compound 3-chloroacrylic acid for growth. The dehalogenases from strain FG41 were purified to homogeneity, and trans-3-chloroacrylic acid dehalogenase (CaaD) was found to be a 50-kDa enzyme composed of different subunits of 8.7 and 7.4 kDa, whereas the cis-3-chloroacrylic acid dehalogenase was an enzyme composed of two or three identical 16-kDa subunits (47). Although large fragments of these dehalogenating enzymes were sequenced, no significant sequence similarities with other protein sequences were found when the different databases were searched in 1992 (47).Whereas most hydrolytic dehalogenase that are active with halogenated aliphatic compounds (so-called halidohydrolases), such as haloalkane dehalogenases (26, 30, 50), haloacetate dehalogenases (15-17), and 2-haloacid dehalogenases (21, 25, 31), are only able to displace halogens bound to sp 3 -hybridized carbon atoms, 3-chloroacrylic acid dehalogenases are unique in that they can cleave the much more stable vinylic carbon-halogen bond, in which the halogen is bound to an sp 2 -hybridized carbon atom. Cleavage of the...

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Section: Discussionmentioning

confidence: 99%

trans -3-Chloroacrylic Acid Dehalogenase from Pseudomonas pavonaceae 170 Shares Structural and Mechanistic Similarities with 4-Oxalocrotonate Tautomerase

2001

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“…Pro-1 can function as a general base under physiological conditions because of its unusually low pK a of 6.4, which is 3 units lower than the pK a of the model compound, proline amide (70). The X-ray structure of 4-OT (71) shows that within a sphere of 9Å radius, Pro-1 is surrounded by hydrophobic residues, creating a site with a low dielectric constant. In addition, Arg-11 and Arg-39 are positioned 11Å and 7Å, respectively, from Pro-1 and are located at opposite sides of the active site, providing binding specificity to the terminal carboxyl groups of the substrate and product.…”

Section: Born or Desolvation Effectmentioning

confidence: 99%

Structural Basis of Perturbed pKa Values of Catalytic Groups in Enzyme Active Sites

2002

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SummaryIn protein and RNA macromolecules, only a limited number of different side-chain chemical groups are available to function as catalysts. The myriad of enzyme-catalyzed reactions results from the ability of most of these groups to function either as nucleophilic, electrophilic, or general acid-base catalysts, and the key to their adapted chemical function lies in their states of protonation. Ionization is determined by the intrinsic pK a of the group and the microenvironment created around the group by the protein or RNA structure, which perturbs its intrinsic pK a to its functional or apparent pK a . These pK a shifts result from interactions of the catalytic group with other fully or partially charged groups as well as the polarity or dielectric of the medium that surrounds it. The electro- Abbreviations: AAD, acetoacetate decarboxylase; AbAld, antibody aldolase; Ala-Race, alanine racemase; hdvAR, hepatitis delta virus antigenomic ribozyme; ArsC, arsenate reductase; AspAT, aspartate aminotransferase; BCX, Bacillus circulans xylanase; BR, ground-state bacteriorhodopsin with all trans retinal, protonated D96, protonated Schiff base, and unprotonated D85; BR-M, excited M-state bacteriorhodopsin with 13-cis retinal, protonated D96, unprotonated Schiff base, and protonated D85; BR-N, excited N-state bacteriorhodopsin with 13-cis retinal, unprotonated D96, protonated Schiff base, and protonated D85; Chy-TFKs, chymotrypsin complexed with various peptidyl trifluoroketones; hmCK, human muscle creatine kinase; DsbA and DsbC, disulfide bond enzymes A and C in E. coli; GalE, UDP-galactose 4-epimerase; GRX, glutaredoxin; HB, hydrogen bond; HPE, hydrophobic environment; KSI, ketosteroid isomerase; LBHB, low-barrier hydrogen bond; NMR, nuclear magnetic resonance; NTα, N-terminus of an α-helix; Nuc/Lv, nucleophile/leaving group; 4-OT, 4-oxalocrotonate tautomerase; PDI, protein disulfide isomerase; PLP, pyridoxal 5 -phosphate; PMP, pyridoxamine 5 -phosphate; blmPTP, bovine liver low molecular weight protein tyrosine phosphatase; hPTP1, human protein tyrosine phosphatase; yPTP, Yersenia protein tyrosine phosphatase; rPTC, ribosomal peptidyl transferase center; RNaseH1, ribonuclease H1; TIM, triosephosphate isomerase; bTRX, bacterial thioredoxin; hTRX, human thioredoxin.

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“…The catalytic mechanism involves a single catalytic base that is the N-terminal proline residue. Two arginine residues interact with the substrate in the active-site region (304,312). Although the HpcD isomerase catalyzes a reaction analogous to that catalyzed by the 4-oxalocrotonate tautomerase of the meta-cleavage pathway of phenol and toluene on a chemically similar substrate, the two enzymes do not have any apparent sequence similarity.…”

Section: Hpc Meta Cleavage Dehydrogenative Routementioning

confidence: 99%

“…Nevertheless, the two isomerases are specific, and each shows a preference for its own substrate. This substrate specificity in the isomerases seems to be determined by steric constraints in the catalytic cleft (304,312).…”

Section: Hpc Meta Cleavage Dehydrogenative Routementioning

confidence: 99%

Biodegradation of Aromatic Compounds by Escherichia coli

Dı́az

Ferrández

Prieto

et al. 2001

Microbiol Mol Biol Rev

324

235

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Although Escherichia coli has long been recognized as the best-understood living organism, little was known about its abilities to use aromatic compounds as sole carbon and energy sources. This review gives an extensive overview of the current knowledge of the catabolism of aromatic compounds by E. coli. After giving a general overview of the aromatic compounds that E. coli strains encounter and mineralize in the different habitats that they colonize, we provide an up-to-date status report on the genes and proteins involved in the catabolism of such compounds, namely, several aromatic acids (phenylacetic acid, 3- and 4-hydroxyphenylacetic acid, phenylpropionic acid, 3-hydroxyphenylpropionic acid, and 3-hydroxycinnamic acid) and amines (phenylethylamine, tyramine, and dopamine). Other enzymatic activities acting on aromatic compounds in E. coli are also reviewed and evaluated. The review also reflects the present impact of genomic research and how the analysis of the whole E. coli genome reveals novel aromatic catabolic functions. Moreover, evolutionary considerations derived from sequence comparisons between the aromatic catabolic clusters of E. coli and homologous clusters from an increasing number of bacteria are also discussed. The recent progress in the understanding of the fundamentals that govern the degradation of aromatic compounds in E. coli makes this bacterium a very useful model system to decipher biochemical, genetic, evolutionary, and ecological aspects of the catabolism of such compounds. In the last part of the review, we discuss strategies and concepts to metabolically engineer E. coli to suit specific needs for biodegradation and biotransformation of aromatics and we provide several examples based on selected studies. Finally, conclusions derived from this review may serve as a lead for future research and applications

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Crystal Structure of 4-Oxalocrotonate Tautomerase Inactivated by 2-Oxo-3-pentynoate at 2.4 Å Resolution: Analysis and Implications for the Mechanism of Inactivation and Catalysis^,

Cited by 73 publications

References 29 publications

trans -3-Chloroacrylic Acid Dehalogenase from Pseudomonas pavonaceae 170 Shares Structural and Mechanistic Similarities with 4-Oxalocrotonate Tautomerase

trans -3-Chloroacrylic Acid Dehalogenase from Pseudomonas pavonaceae 170 Shares Structural and Mechanistic Similarities with 4-Oxalocrotonate Tautomerase

Structural Basis of Perturbed pKa Values of Catalytic Groups in Enzyme Active Sites

Biodegradation of Aromatic Compounds by Escherichia coli

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Crystal Structure of 4-Oxalocrotonate Tautomerase Inactivated by 2-Oxo-3-pentynoate at 2.4 Å Resolution: Analysis and Implications for the Mechanism of Inactivation and Catalysis,

Cited by 73 publications

References 29 publications

trans -3-Chloroacrylic Acid Dehalogenase from Pseudomonas pavonaceae 170 Shares Structural and Mechanistic Similarities with 4-Oxalocrotonate Tautomerase

trans -3-Chloroacrylic Acid Dehalogenase from Pseudomonas pavonaceae 170 Shares Structural and Mechanistic Similarities with 4-Oxalocrotonate Tautomerase

Structural Basis of Perturbed pKa Values of Catalytic Groups in Enzyme Active Sites

Biodegradation of Aromatic Compounds by Escherichia coli

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Crystal Structure of 4-Oxalocrotonate Tautomerase Inactivated by 2-Oxo-3-pentynoate at 2.4 Å Resolution: Analysis and Implications for the Mechanism of Inactivation and Catalysis^,