A comparative study of fragment screening methods on the p38α kinase: new methods, new insights

Pollack, Scott J.; Beyer, Kim S.; Lock, Christopher; Müller, Ilse; Sheppard, David N.; Lipkin, M. A.; Hardick, David J.; Blurton, Peter; Leonard, Philip; Hubbard, Paul A.; Todd, Daniel E.; Richardson, Christine M.; Ahrens, Tom; Baader, Manuel; Hafenbradl, Doris; Hilyard, Kate; Bürli, Roland W.

doi:10.1007/s10822-011-9454-9

Cited by 32 publications

(25 citation statements)

References 17 publications

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“…Compared to reports in literature using other techniques (SPR, NMR and fluorescence) 27, 28 , this is a higher proportion of fragment hits yielding X-ray structures. There are several possible explanations for the high proportion of crystallizable fragment hits seen here.…”

Section: Discussionmentioning

confidence: 67%

Identification and Optimization of PDE10A Inhibitors Using Fragment-Based Screening by Nanocalorimetry and X-ray Crystallography

et al. 2014

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Fragment-based lead discovery (FBLD) is a technique in which, small, low-complexity chemical fragments of 6 to 15 heavy atoms are screened for binding to or inhibiting activity of the target. Hits are then linked and/ or elaborated into tightly binding ligands, ideally yielding early lead compounds for drug discovery. Calorimetry provides a label-free method to assay binding and enzymatic activity that is unaffected by the spectroscopic properties of the sample. Conventional microcalorimetry is hampered by requiring large quantities of reagents and long measurement times. Nanocalorimeters can overcome these limitations of conventional isothermal titration calorimetry. Here we use enthalpy arrays, which are arrays of nanocalorimeters, to perform an enzyme activity-based fragment screen for competitive inhibitors of phosphodiesterase 10A (PDE10A). Two dozen fragments with KI <2 mM were identified and moved to crystal soaking trials. All soak experiments yielded high resolution diffraction with two-thirds of the fragments yielding high-resolution co-crystal structures with PDE10A. The structural information was used to elaborate fragment hits, yielding leads with KI <1 µM. This study shows how array calorimetry can be used as a prescreening method for fragment-based lead discovery with enzyme targets and paired successfully with an x-ray crystallography secondary screen.

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Section: Discussionmentioning

confidence: 67%

Identification and Optimization of PDE10A Inhibitors Using Fragment-Based Screening by Nanocalorimetry and X-ray Crystallography

et al. 2014

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“…Ligand-binding alters this shell in a way that measurably changes the molecules' thermophoretic movement293031. MST yields results that are comparable to SPR and other binding assays32. However, unlike SPR or other surface-based techniques, MST does not require immobilization.…”

Section: Resultsmentioning

confidence: 99%

Structure and function analyses of the purified GPCR human vomeronasal type 1 receptor 1

Corin

Philipp

Geißler

et al. 2011

Sci Rep

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The vomeronasal system is one of several fine-tuned scent-detecting signaling systems in mammals. However, despite significant efforts, how these receptors detect scent remains an enigma. One reason is the lack of sufficient purified receptors to perform detailed biochemical, biophysical and structural analyses. Here we report the ability to express and purify milligrams of purified, functional human vomeronasal receptor hVN1R1. Circular dichroism showed that purified hVN1R1 had an alpha-helical structure, similar to that of other GPCRs. Microscale thermophoresis showed that hVN1R1 bound its known ligand myrtenal with an EC50 ∼1 µM. This expression system can enable structural and functional analyses towards understanding how mammalian scent detection works.

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“…The principles of FBDD are based on three key tenets. The first tenet is that a small number of low molecular weight compounds e (known as 'fragments') can represent large areas of chemical space (Pollack et al, 2011). The second tenet is that as the molecular weight and thus complexity of a molecule increases, the probability of an unfavourable interaction also increases (Hann et al, 2001).…”

Section: Introduction To Fragment Screeningmentioning

confidence: 99%

Fragment screening by SPR and advanced application to GPCRs

Shepherd

Hopkins

Navrátilová

2014

Progress in Biophysics and Molecular Biology

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Surface plasmon resonance (SPR) is one of the primary biophysical methods for the screening of low molecular weight 'fragment' libraries, due to its low protein consumption and 'label-free' methodology. SPR biosensor interaction analysis is employed to both screen and confirm the binding of compounds in fragment screening experiments, as it provides accurate information on the affinity and kinetics of molecular interactions. The most advanced application of the use of SPR for fragment screening is against membrane protein drug targets, such G-protein coupled receptors (GPCRs). Biophysical GPCR assays using SPR have been validated with pharmacological measurements approximate to cell-based methods, yet provide the advantage of biophysical methods in their ability to measure the weak affinities of low molecular weight fragments. A number of SPR fragment screens against GPCRs have now been disclosed in the literature. SPR fragment screening is proving versatile to screen both thermostabilised GPCRs and solubilised wild type receptors. In this chapter, we discuss the state-of-the-art in GPCR fragment screening by SPR and the technical considerations in performing such experiments.

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A comparative study of fragment screening methods on the p38α kinase: new methods, new insights

Cited by 32 publications

References 17 publications

Identification and Optimization of PDE10A Inhibitors Using Fragment-Based Screening by Nanocalorimetry and X-ray Crystallography

Identification and Optimization of PDE10A Inhibitors Using Fragment-Based Screening by Nanocalorimetry and X-ray Crystallography

Structure and function analyses of the purified GPCR human vomeronasal type 1 receptor 1

Fragment screening by SPR and advanced application to GPCRs

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