One Question, Multiple Answers: Biochemical and Biophysical Screening Methods Retrieve Deviating Fragment Hit Lists

Schiebel, J.; Radeva, Nedyalka; Köster, Helene; Metz, A.; Krotzky, Timo; Kuhnert, Maren; Diederich, Wibke E.; Heine, A.; Neumann, Lars; Atmanène, Cédric; Roecklin, Dominique; Vivat-Hannah, Valérie; Renaud, Jean‐Paul; Meinecke, Robert; Schlinck, Nina; Sitte, Astrid; Popp, Franziska; Zeeb, Markus; Klebe, G.

doi:10.1002/cmdc.201500267

Cited by 57 publications

(109 citation statements)

References 49 publications

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“…35 The highest hit rate was found for biochemical screening (17%) followed by NMR (11%) and thermal shift assay (8%). It is important to note, however, that the authors neither The different assays were performed under similar conditions including the buffers.…”

Section: Methodsmentioning

confidence: 98%

Design Principles for Fragment Libraries: Maximizing the Value of Learnings from Pharma Fragment-Based Drug Discovery (FBDD) Programs for Use in Academia

et al. 2016

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Fragment-based drug discovery (FBDD) is well suited for discovering both drug leads and chemical probes of protein function: it can cover broad swaths of chemical space and allows the use of creative chemistry. FBDD is widely implemented for lead discovery in industry, but is sometimes used less systematically in academia. Design principles and implementation approaches for fragment libraries are continually evolving, and the lack of up-to-date guidance may prevent more effective application of FBDD in academia. This Perspective explores many of the theoretical, practical, and strategic considerations that occur within FBDD programs, including the optimal size, complexity, physicochemical profile, and shape profile of fragments in FBDD libraries, as well as compound storage, evaluation, and screening technologies. This compilation of industry experience in FBDD will hopefully be useful for those pursuing FBDD in academia.Rules are for the obedience of fools and the guidance of wise men.Harry Day, Royal Air Force (1898-1977

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Section: Methodsmentioning

confidence: 98%

Design Principles for Fragment Libraries: Maximizing the Value of Learnings from Pharma Fragment-Based Drug Discovery (FBDD) Programs for Use in Academia

et al. 2016

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“…Dies schränkt den Einsatz von biochemischen Aktivitätsassays,d ie auf spektroskopischen Methoden wie Fluoreszenz-oder UV/Vis-Spektroskopie beruhen, deutlich ein. [24] Biophysikalische Methoden wie die Biolayer-Interferometrie sind bezüglich Assayinterferenzen weniger stçranfällig und daher für fragmentbasiertes Screening besser geeignet. [25] Um die Eignung unserer SirReal-Sonde in Kombination mit der Biolayer-Interferometrie für fragmentbasierte Screeningansätze zu prüfen, testeten wir Fragmente von SirReal2 (2) [26] zu identifizieren und genomweite Bindungsprofile für Sirt2 durch Chem-seq [27] zu erstellen.…”

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Strukturbasierte Entwicklung einer Affinitätssonde für Sirtuin 2

et al. 2015

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“…26–28 The use of MST is increasingly being reported in fragment-based drug discovery, 23,24,30–33 including kinases such as p38α 30 and MEK1, 31 and the bromodomain BRD9. 32 In both the MEK1 study by Sanofi in collaboration with NanoTemper and the BRD9 study by Boehringer Ingelheim, MST was used to confirm the binding of fragments identified by SPR and DSF, as well as to identify additional hits not detected by the other techniques.…”

Section: Microscale Thermophoresismentioning

confidence: 99%

Using Microscale Thermophoresis to Characterize Hits from High-Throughput Screening: A European Lead Factory Perspective

2018

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High-throughput screening (HTS) is a proven method for discovering new lead matter for drug discovery and chemical biology. To maximize the likelihood of identifying genuine binders to a molecular target, and avoid wasting resources following up compounds with unproductive/nonspecific mechanisms of action, it is important to employ a range of assays during an HTS campaign that build confidence of target engagement for hit compounds. Biophysical methods that measure direct target/compound engagement have established themselves as key techniques in generating this confidence, and they are now integral to the latter stages of HTS triage at the European Lead Factory (ELF). One relatively new technique that the ELF is using is microscale thermophoresis (MST), which measures the differences in rate of movement through a temperature gradient that are caused when single molecular species form complexes. Here we provide an overview of the MST assay development workflow that the ELF employs and a perspective of our experience to date of using MST to triage the output of HTS campaigns and how it compares and contrasts with the use of other biophysical techniques.

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One Question, Multiple Answers: Biochemical and Biophysical Screening Methods Retrieve Deviating Fragment Hit Lists

Cited by 57 publications

References 49 publications

Design Principles for Fragment Libraries: Maximizing the Value of Learnings from Pharma Fragment-Based Drug Discovery (FBDD) Programs for Use in Academia

Design Principles for Fragment Libraries: Maximizing the Value of Learnings from Pharma Fragment-Based Drug Discovery (FBDD) Programs for Use in Academia

Strukturbasierte Entwicklung einer Affinitätssonde für Sirtuin 2

Using Microscale Thermophoresis to Characterize Hits from High-Throughput Screening: A European Lead Factory Perspective

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