Mutational and x-ray crystallographic analysis of the interaction of dihomo-y-linolenic acid with prostaglandin endoperoxide H synthases.

Thuresson, E D; Malkowski, M G; Lakkides, K M; Rieke, C J; Mulichak, A M; Ginell, S; Garavito, R M; Smith, W L

Title: Mutational and x-ray crystallographic analysis of the interaction of dihomo-y-linolenic acid with prostaglandin endoperoxide H synthases.

Journal Article · Sun Mar 30 00:00:00 EST 2003 · J. Biol. Chem.

OSTI ID:949279

Thuresson, E D; Malkowski, M G; Lakkides, K M; Rieke, C J; Mulichak, A M; Ginell, S; Garavito, R M; Smith, W L

Prostaglandin endoperoxide H synthases-1 and -2 (PGHSs) catalyze the committed step in prostaglandin biosynthesis. Both isozymes can oxygenate a variety of related polyunsaturated fatty acids. We report here the x-ray crystal structure of dihomo-{gamma}-linolenic acid (DHLA) in the cyclooxygenase site of PGHS-1 and the effects of active site substitutions on the oxygenation of DHLA, and we compare these results to those obtained previously with arachidonic acid (AA). DHLA is bound within the cyclooxygenase site in the same overall L-shaped conformation as AA. C-1 and C-11 through C-20 are in the same positions for both substrates, but the positions of C-2 through C-10 differ by up to 1.74 Angstroms. In general, substitutions of active site residues caused parallel changes in the oxygenation of both AA and DHLA. Two significant exceptions were Val-349 and Ser-530. A V349A substitution caused an 800-fold decrease in the Vmax/Km for DHLA but less than a 2-fold change with AA; kinetic evidence indicates that C-13 of DHLA is improperly positioned with respect to Tyr-385 in the V349A mutant thereby preventing efficient hydrogen abstraction. Val-349 contacts C-5 of DHLA and appears to serve as a structural bumper positioning the carboxyl half of DHLA, which, in turn, positions properly the omega -half of this substrate. A V349A substitution in PGHS-2 has similar, minor effects on the rates of oxygenation of AA and DHLA. Thus, Val-349 is a major determinant of substrate specificity for PGHS-1 but not for PGHS-2. Ser-530 also influences the substrate specificity of PGHS-1; an S530T substitution causes 40- and 750-fold decreases in oxygenation efficiencies for AA and DHLA, respectively.

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Research Organization:: Argonne National Lab. (ANL), Argonne, IL (United States)

Sponsoring Organization:: USDOE Office of Science (SC); National Institutes of Health (NIH)

DOE Contract Number:: DE-AC02-06CH11357

OSTI ID:: 949279

Report Number(s):: ANL/BIO/JA-39502; JBCHA3; TRN: US201012%%77

Journal Information:: J. Biol. Chem., Vol. 276, Issue 13 ; Mar. 30, 2003; ISSN 0021-9258

Country of Publication:: United States

Language:: ENGLISH

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08 HYDROGEN
36 MATERIALS SCIENCE
ARACHIDONIC ACID
BIOSYNTHESIS
CARBOXYLIC ACIDS
CRYSTAL STRUCTURE
HYDROGEN
KINETICS
MUTANTS
POSITIONING
PROSTAGLANDINS
RESIDUES
SPECIFICITY
SUBSTRATES

Title: Mutational and x-ray crystallographic analysis of the interaction of dihomo-y-linolenic acid with prostaglandin endoperoxide H synthases.

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