2002
DOI: 10.1096/fj.01-1017fje
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Crystal structures of leukotriene A4 hydrolase in complex with captopril and two competitive tight‐binding inhibitors

Abstract: Leukotriene (LT) A4 hydrolase/aminopeptidase is a bifunctional zinc enzyme that catalyzes the final step in the biosynthesis of LTB4, a potent chemoattractant and immune modulating lipid mediator. Here, we report a high-resolution crystal structure of LTA4 hydrolase in complex with captopril, a classical inhibitor of the zinc peptidase angiotensin-converting enzyme. Captopril makes few interactions with the protein, but its free thiol group is bound to the zinc, apparently accounting for most of its inhibitory… Show more

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Cited by 69 publications
(67 citation statements)
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“…This soluble enzyme converts LTA 4 into LTB 4 and thus provides an alternative fate for the product of the 5-LOX reaction. The crystal structure of LTA 4 hydrolase confirmed the prediction from sequence alignments that it is a member of the M1 amino peptidase superfamily (37,38). These are zinc-containing amino peptidases typified by thermolysin.…”
Section: Protein Structuressupporting
confidence: 68%
See 1 more Smart Citation
“…This soluble enzyme converts LTA 4 into LTB 4 and thus provides an alternative fate for the product of the 5-LOX reaction. The crystal structure of LTA 4 hydrolase confirmed the prediction from sequence alignments that it is a member of the M1 amino peptidase superfamily (37,38). These are zinc-containing amino peptidases typified by thermolysin.…”
Section: Protein Structuressupporting
confidence: 68%
“…Consequently, regulation of pathway flux can be executed by the subcellular targeting of key enzymes. For example, as described below, targeting of 5-LOX to the outer nuclear membrane is thought to promote the formation of the cysteinyl-LTs, whereas 5-LOX targeting to the inner nuclear membrane results in the production of LTB 4 (37,38).…”
Section: Compartmentalizationmentioning
confidence: 99%
“…In keeping with these data is the model for binding of an arginyl tripeptide substrate to LTA4H. In this model, Tyr378, the residue corresponding to Phe544 in IRAP, plays a role in defining the S1 and S2Ј subsites of the active site (Thunnissen et al, 2002).…”
Section: Discussionmentioning
confidence: 99%
“…One patch of the cavity is hydrophilic, with Gln-134, Asp-375, and the hydroxyl of Tyr-267 clustering together. This cavity was probed by structural determination of complexes between LTA4H and specific, active site-directed inhibitors, some of which have been designed as LTA 4 mimics (35). Indeed, the hydrophobic tail of the inhibitors, corresponding to the fatty acid backbone of LTA 4 , is buried into the narrow hydrophobic pocket, strongly indicating that it functions as a substrate binding cavity (Fig.…”
Section: Crystal Structure Of Lta 4 Hydrolasementioning
confidence: 99%