Litcius/Paper detail

Crystal structure of pathogenic Staphylococcus aureus lipase complex with the anti-obesity drug orlistat

Kengo Kitadokoro, M. Tanaka, Takaaki Hikima, Yukiko Okuno, Masaki Yamamoto, Shigeki Kamitani

2020Scientific Reports32 citationsDOIOpen Access PDF

Abstract

Staphylococcus aureus lipase (SAL), a triacylglycerol esterase, is an important virulence factor and may be a therapeutic target for infectious diseases. Herein, we determined the 3D structure of native SAL, the mutated S116A inactive form, and the inhibitor complex using the anti-obesity drug orlistat to aid in drug development. The determined crystal structures showed a typical α/β hydrolase motif with a dimeric form. Fatty acids bound near the active site in native SAL and inactive S116A mutant structures. We found that orlistat potently inhibits SAL activity, and it covalently bound to the catalytic Ser116 residue. This is the first report detailing orlistat-lipase binding. It provides structure-based information on the production of potent anti-SAL drugs and lipase inhibitors. These results also indicated that orlistat can be repositioned to treat bacterial diseases.

Topics & Concepts

OrlistatLipaseStaphylococcus aureusChemistryDrugHydrolaseEsteraseBiochemistryEnzymeBiologyPharmacologyObesityBacteriaGeneticsEndocrinologyWeight lossEnzyme Catalysis and ImmobilizationEnzyme Structure and FunctionPlant biochemistry and biosynthesis