Towards mimicking short linear peptide motifs: identification of new mixed α,β-peptidomimetic ligands for SLAM-Associated Protein (SAP) by confocal on-bead screening

Hintersteiner, Martin; Knox, Andrew J. S.; Mudd, Gemma; Auer, Manfred

doi:10.1007/s12154-011-0071-9

Cited by 7 publications

(7 citation statements)

References 26 publications

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“…PS/PS relies on including a generic tagging site for post-screening in situ labeling of hit compounds with a fluorescent dye and subsequent miniaturized affinity determination in solution. [21,22] The second approach uses a chemically stable UVfluorophore, AIDA, as a permanent tag introduced on each compound during library synthesis. [23,24] The indazole dye, AIDA, is then used as mass-tag for decoding and as a tracer for affinity determination.…”

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confidence: 99%

Identification and X‐ray Co‐crystal Structure of a Small‐Molecule Activator of LFA‐1‐ICAM‐1 Binding

et al. 2014

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Stabilization of protein–protein interactions by small molecules is a concept with few examples reported to date. Herein we describe the identification and X-ray co-crystal structure determination of IBE-667, an ICAM-1 binding enhancer for LFA-1. IBE-667 was designed based on the SAR information obtained from an on-bead screen of tagged one-bead one-compound combinatorial libraries by confocal nanoscanning and bead picking (CONA). Cellular assays demonstrate the activity of IBE-667 in promoting the binding of LFA-1 on activated immune cells to ICAM-1.

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confidence: 99%

Identification and X‐ray Co‐crystal Structure of a Small‐Molecule Activator of LFA‐1‐ICAM‐1 Binding

et al. 2014

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“…However, modern Chemical Biology research, which uses compounds as tools for understating biological systems increasingly utilizes post‐synthesis tagging methods . Also, the use of combinatorial libraries for on‐bead screening or similar display technologies requires that the final compounds can be fully deprotected while it still remains linked to the solid surface. These requirements for flexibility and increased chemical compatibility have led to the development of more sophisticated linker concepts, such as photo‐cleavable linkers and safety–catch linkers .…”

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confidence: 99%

Facile Synthesis of a Next Generation Safety‐Catch Acid‐Labile Linker, SCAL‐2, Suitable for Solid‐Phase Synthesis, On‐Support Display and for Post‐Synthesis Tagging

Portal¹,

Hintersteiner

Barbeau

et al. 2017

ChemistrySelect

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The SCAL linker, a safety catch linker, is amongst the most versatile linkers for solid phase synthesis. It was originally described in 1991 by Pátek and Lebl. Yet, its application has been hindered by the low yields of published synthetic routes. Over time, the exceptional versatility of this linker has been demonstrated in several applications of advanced solid phase synthesis of peptides and peptidomimetics. Recently, an updated synthesis of the original linker has also been presented at the 22nd American Peptide Symposium, comprising 10 steps. Herein, the design and synthesis of a next generation SCAL linker, SCAL‐2, is reported. SCAL‐2 features a simplified molecular architecture, which allows for a more efficient synthesis in 8 steps with superior yields. Both linkers, SCAL and SCAL‐2 are compared in terms of their cleavage properties adding valuable information on how to best utilize the versatility of these linkers for solid phase synthesis.

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“…13 This very efficient initial screening step can then be combined with different follow-up assays for further characterization and ranking of individual hit beads before resources are committed to the resynthesis of screening hits. 14,15 One of the major hurdles for a wider application of on-bead screening is the lack of simple, automated screening platforms. In its simplest implementation, a fluorescently tagged protein is incubated with library beads to assay surface binding to specific bead-immobilized compounds.…”

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confidence: 99%

“…Thus, the amount of chemical substances required for screening and the corresponding assay volumes are among the lowest for industrial screening procedures . This very efficient initial screening step can then be combined with different follow-up assays for further characterization and ranking of individual hit beads before resources are committed to the resynthesis of screening hits. , …”

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A Wide-Field Fluorescence Microscope Extension for Ultrafast Screening of One-Bead One-Compound Libraries Using a Spectral Image Subtraction Approach

Heusermann

Ludin²,

Pham

et al. 2016

ACS Comb. Sci.

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The increasing involvement of academic institutions and biotech companies in drug discovery calls for cost-effective methods to identify new bioactive molecules. Affinity-based on-bead screening of combinatorial one-bead one-compound libraries combines a split-mix synthesis design with a simple protein binding assay operating directly at the bead matrix. However, one bottleneck for academic scale on-bead screening is the unavailability of a cheap, automated, and robust screening platform that still provides a quantitative signal related to the amount of target protein binding to individual beads for hit bead ranking. Wide-field fluorescence microscopy has long been considered unsuitable due to significant broad spectrum autofluorescence of the library beads in conjunction with low detection sensitivity. Herein, we demonstrate how such a standard microscope equipped with LED-based excitation and a modern CMOS camera can be successfully used for selecting hit beads. We show that the autofluorescence issue can be overcome by an optical image subtraction approach that yields excellent signal-to-noise ratios for the detection of bead-associated target proteins. A polymer capillary attached to a semiautomated bead-picking device allows the operator to efficiently isolate individual hit beads in less than 20 s. The system can be used for ultrafast screening of >200,000 bead-bound compounds in 1.5 h, thereby making high-throughput screening accessible to a wider group within the scientific community.

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Towards mimicking short linear peptide motifs: identification of new mixed α,β-peptidomimetic ligands for SLAM-Associated Protein (SAP) by confocal on-bead screening

Cited by 7 publications

References 26 publications

Identification and X‐ray Co‐crystal Structure of a Small‐Molecule Activator of LFA‐1‐ICAM‐1 Binding

Identification and X‐ray Co‐crystal Structure of a Small‐Molecule Activator of LFA‐1‐ICAM‐1 Binding

Facile Synthesis of a Next Generation Safety‐Catch Acid‐Labile Linker, SCAL‐2, Suitable for Solid‐Phase Synthesis, On‐Support Display and for Post‐Synthesis Tagging

A Wide-Field Fluorescence Microscope Extension for Ultrafast Screening of One-Bead One-Compound Libraries Using a Spectral Image Subtraction Approach

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