Multistage Screening Reveals Chameleon Ligands of the Human Farnesyl Pyrophosphate Synthase: Implications to Drug Discovery for Neurodegenerative Diseases

Schutter, Joris W. De; Park, Jaeok; Leung, Chun Yuen; Gormley, Patrick; Lin, Yih‐Shyan; Hu, Zheping; Berghuis, Albert M.; Poirier, Judes; Tsantrizos, Youla S.

doi:10.1021/jm500629e

Cited by 29 publications

(99 citation statements)

References 52 publications

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“…The one-site-binding pattern observed here is a consequence of the enzyme closure, which renders the allosteric pocket inaccessible to the substrates. Analogous results demonstrating the biased binding (that is, binding exclusively to the allylic substrate site in the presence of Mg 2+ ) have been confirmed crystallographically with allosteric BPs912. In contrast to the binding of DMAPP and GPP, FPP binding was not affected by Mg 2+ (Table 2).…”

Section: Resultssupporting

confidence: 59%

“…Interestingly, the binding mode of FPP differs from those of the allosteric BPs reported earlier910. Their pyrophosphate/BP groups interact with the enzyme differently from one another and do not overlap when superimposed (Supplementary Fig.…”

Section: Resultsmentioning

confidence: 83%

“…2b). Direct interaction between anionic molecules at this site has been observed multiple times91011 and suggests that their charges are neutralized by surrounding protein residues. The tail of FPP extends deep into the allosteric pocket, making tight van der Waals contacts with the protein surface (Fig.…”

Section: Resultsmentioning

confidence: 93%

“…However, neither cholesterol and bile acids (downstream metabolites) nor nucleotides and their analogues inhibited the enzyme8. More recently, our own efforts identified a different series of non-BP inhibitors targeting the same pocket910. Here we discovered that certain BPs—all of them with bulky lipophilic side chains—could bind to this pocket.…”

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confidence: 92%

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Human farnesyl pyrophosphate synthase is allosterically inhibited by its own product

et al. 2017

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Farnesyl pyrophosphate synthase (FPPS) is an enzyme of the mevalonate pathway and a well-established therapeutic target. Recent research has focused around a newly identified druggable pocket near the enzyme's active site. Pharmacological exploitation of this pocket is deemed promising; however, its natural biological function, if any, is yet unknown. Here we report that the product of FPPS, farnesyl pyrophosphate (FPP), can bind to this pocket and lock the enzyme in an inactive state. The Kd for this binding is 5–6 μM, within a catalytically relevant range. These results indicate that FPPS activity is sensitive to the product concentration. Kinetic analysis shows that the enzyme is inhibited through FPP accumulation. Having a specific physiological effector, FPPS is a bona fide allosteric enzyme. This allostery offers an exquisite mechanism for controlling prenyl pyrophosphate levels in vivo and thus contributes an additional layer of regulation to the mevalonate pathway.

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Section: Resultssupporting

confidence: 59%

Section: Resultsmentioning

confidence: 83%

Section: Resultsmentioning

confidence: 93%

mentioning

confidence: 92%

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Human farnesyl pyrophosphate synthase is allosterically inhibited by its own product

et al. 2017

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“…Following these initial reports, in silico screening identified bisamidine-type inhibitors of hFPPS (e.g., 17 ) (Lindert et al, 2013), although the binding mode of these compounds has also not been reported. In our own efforts, multistage biochemical and structural screening led to the discovery of thienopyrimidine analogs (e.g., 18 ) that bind to the same allosteric pocket as compound 13 and exhibit equivalent in vitro potency (De Schutter et al, 2014). …”

Section: Isoprenoids Fpps/ggpps and Neurodegeneration—the Current Hypmentioning

confidence: 99%

Human isoprenoid synthase enzymes as therapeutic targets

et al. 2014

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In the human body, the complex biochemical network known as the mevalonate pathway is responsible for the biosynthesis of all isoprenoids, which consists of a vast array of metabolites that are vital for proper cellular functions. Two key isoprenoids, farnesyl pyrophosphate (FPP) and geranylgeranyl pyrophosphate (GGPP) are responsible for the post-translational prenylation of small GTP-binding proteins, and serve as the biosynthetic precursors to numerous other biomolecules. The down-stream metabolite of FPP and GGPP is squalene, the precursor to steroids, bile acids, lipoproteins, and vitamin D. In the past, interest in prenyl synthase inhibitors focused mainly on the role of the FPP in lytic bone diseases. More recently pre-clinical and clinical studies have strongly implicated high levels of protein prenylation in a plethora of human diseases, including non-skeletal cancers, the progression of neurodegenerative diseases and cardiovascular diseases. In this review, we focus mainly on the potential therapeutic value of down-regulating the biosynthesis of FPP, GGPP, and squalene. We summarize the most recent drug discovery efforts and the structural data available that support the current on-going studies.

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Gezielte Anreicherung von Wirkstoffen am Knochen am Beispiel von allosterischen FPPS‐Inhibitoren

et al. 2015

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Multistage Screening Reveals Chameleon Ligands of the Human Farnesyl Pyrophosphate Synthase: Implications to Drug Discovery for Neurodegenerative Diseases

Cited by 29 publications

References 52 publications

Human farnesyl pyrophosphate synthase is allosterically inhibited by its own product

Human farnesyl pyrophosphate synthase is allosterically inhibited by its own product

Human isoprenoid synthase enzymes as therapeutic targets

Gezielte Anreicherung von Wirkstoffen am Knochen am Beispiel von allosterischen FPPS‐Inhibitoren

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