Interactions at the Dimer Interface Influence the Relative Efficiencies for Purine Nucleotide Synthesis and Pyrophosphorolysis in a Phosphoribosyltransferase

Canyuk, Bhutorn; Medrano, Francisco J; Wenck, MaryAnne; Focia, Pamela J; Eakin, Ann E; Craig, III, Sydney P

Title: Interactions at the Dimer Interface Influence the Relative Efficiencies for Purine Nucleotide Synthesis and Pyrophosphorolysis in a Phosphoribosyltransferase

Journal Article · Fri Mar 05 00:00:00 EST 2010 · J. Mol. Biol.

OSTI ID:1008745

Canyuk, Bhutorn; Medrano, Francisco J; Wenck, MaryAnne; Focia, Pamela J; Eakin, Ann E; Craig, III, Sydney P ^[1]

Enzymes that salvage 6-oxopurines, including hypoxanthine phosphoribosyltransferases (HPRTs), are potential targets for drugs in the treatment of diseases caused by protozoan parasites. For this reason, a number of high-resolution X-ray crystal structures of the HPRTs from protozoa have been reported. Although these structures did not reveal why HPRTs need to form dimers for catalysis, they revealed the existence of potentially relevant interactions involving residues in a loop of amino acid residues adjacent to the dimer interface, but the contributions of these interactions to catalysis remained poorly understood. The loop, referred to as active-site loop I, contains an unusual non-proline cis-peptide and is composed of residues that are structurally analogous with Leu67, Lys68, and Gly69 in the human HPRT. Functional analyses of site-directed mutations (K68D, K68E, K68N, K68P, and K68R) in the HPRT from Trypanosoma cruzi, etiologic agent of Chagas disease, show that the side-chain at position 68 can differentially influence the K{sub m} values for all four substrates as well as the k{sub cat} values for both IMP formation and pyrophosphorolysis. Also, the results for the K68P mutant are inconsistent with a cis-trans peptide isomerization-assisted catalytic mechanism. These data, together with the results of structural studies of the K68R mutant, reveal that the side-chain of residue 68 does not participate directly in reaction chemistry, but it strongly influences the relative efficiencies for IMP formation and pyrophosphorolysis, and the prevalence of lysine at position 68 in the HPRT of the majority of eukaryotes is consistent with there being a biological role for nucleotide pyrophosphorolysis.

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Research Organization:: Argonne National Lab. (ANL), Argonne, IL (United States). Advanced Photon Source (APS)

Sponsoring Organization:: USDOE

OSTI ID:: 1008745

Journal Information:: J. Mol. Biol., Vol. 335, Issue (4) ; 01, 2004; ISSN 0022-2836

Country of Publication:: United States

Language:: ENGLISH

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Related Subjects

36 MATERIALS SCIENCE
AMINO ACIDS
CATALYSIS
CRYSTAL STRUCTURE
DIMERS
ENZYMES
FUNCTIONALS
HYPOXANTHINE PHOSPHORIBOSYLTRANSFERASE
LYSINE
MUTANTS
MUTATIONS
NUCLEOTIDES
PARASITES
PEPTIDES
PROTOZOA
PURINES
RESIDUES
SUBSTRATES
SYNTHESIS
TARGETS
TRYPANOSOMA

Title: Interactions at the Dimer Interface Influence the Relative Efficiencies for Purine Nucleotide Synthesis and Pyrophosphorolysis in a Phosphoribosyltransferase

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