Structure Report for: 5W95

Goins, C.M., Schreidah, C.M., Ronning, D.R.: Lacks cutinase activity has thioesterase and Phospholipase A (PLA) activity

Title: Structural basis for lipid binding and mechanism of the Mycobacterium tuberculosis Rv3802 phospholipase
Goins CM, Schreidah CM, Dajnowicz S, Ronning DR
Ref: Journal of Biological Chemistry, 293:1363, 2018 : PubMed
Abstract


ESTHER: Goins_2018_J.Biol.Chem_293_1363
PubMedSearch: Goins 2018 J.Biol.Chem 293 1363
PubMedID: 29247008
Gene_locus related to this paper: myctu-Rv3802c
Inhibitor(s) related to this paper: Pentaethylene-glycol

Abstract

The Mycobacterium tuberculosis rv3802c gene encodes an essential enzyme with thioesterase and phospholipase A activity. Overexpression of Rv3802 orthologs in Mycobacterium smegmatis and Corynebacterium glutamicum increases mycolate content and decreases glycerophospholipids. Although a role in modulating the lipid composition of the unique mycomembrane has been proposed, the true biological function of Rv3802 remains uncertain. In this study, we present the first M. tuberculosis Rv3802 X-ray crystal structure, solved to 1.7 A resolution. On the basis of the binding of PEG molecules to Rv3802, we identified its lipid-binding site and the structural basis for phosphatidyl-based substrate binding and phospholipase A activity. We found that movement of the alpha8-helix affords lipid binding and is required for catalytic turnover through covalent tethering. We gained insights into the mechanism of acyl hydrolysis by observing differing arrangements of PEG and water molecules within the active site. This study provides structural insights into biological function and facilitates future structure-based drug design toward Rv3802.