Structure and Mechanism of the Farnesyl Diphosphate Synthase from Trypanosoma cruzi: Implications for Drug Design

Gabelli, S; McLellan, J; Montalvetti, A; Oldfield, E; Docampo, R; Amzel, L

doi:10.1002/prot.20754

Title: Structure and Mechanism of the Farnesyl Diphosphate Synthase from Trypanosoma cruzi: Implications for Drug Design

Journal Article · Sun Jan 01 00:00:00 EST 2006 · Proteins Struc. Func. Bioinformatics

DOI:https://doi.org/10.1002/prot.20754· OSTI ID:914269

Gabelli, S; McLellan, J; Montalvetti, A; Oldfield, E; Docampo, R; Amzel, L

Typanosoma cruzi, the causative agent of Chagas disease, has recently been shown to be sensitive to the action of the bisphosphonates currently used in bone resorption therapy. These compounds target the mevalonate pathway by inhibiting farnesyl diphosphate synthase (farnesyl pyrophosphate synthase, FPPS), the enzyme that condenses the diphosphates of C{sub 5} alcohols (isopentenyl and dimethylallyl) to form C{sub 10} and C{sub 15} diphosphates (geranyl and farnesyl). The structures of the T. cruzi FPPS (TcFPPS) alone and in two complexes with substrates and inhibitors reveal that following binding of the two substrates and three Mg2+ ions, the enzyme undergoes a conformational change consisting of a hinge-like closure of the binding site. In this conformation, it would be possible for the enzyme to bind a bisphosphonate inhibitor that spans the sites usually occupied by dimethylallyl diphosphate (DMAPP) and the homoallyl moiety of isopentenyl diphosphate. This observation may lead to the design of new, more potent anti-trypanosomal bisphosphonates, because existing FPPS inhibitors occupy only the DMAPP site. In addition, the structures provide an important mechanistic insight: after its formation, geranyl diphosphate can swing without leaving the enzyme, from the product site to the substrate site to participate in the synthesis of farnesyl diphosphate.

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Research Organization:: Brookhaven National Lab. (BNL), Upton, NY (United States). National Synchrotron Light Source

Sponsoring Organization:: Doe - Office Of Science

DOE Contract Number:: DE-AC02-98CH10886

OSTI ID:: 914269

Report Number(s):: BNL-78837-2007-JA; TRN: US200809%%19

Journal Information:: Proteins Struc. Func. Bioinformatics, Vol. 62, Issue 1

Country of Publication:: United States

Language:: English

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59 BASIC BIOLOGICAL SCIENCES
ALCOHOLS
CONFORMATIONAL CHANGES
DESIGN
ENZYMES
PYROPHOSPHATES
SUBSTRATES
SYNTHESIS
THERAPY
TRYPANOSOMA
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Title: Structure and Mechanism of the Farnesyl Diphosphate Synthase from Trypanosoma cruzi: Implications for Drug Design

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