Literature DB >> 19397369

On-bead screening of combinatorial libraries: reduction of nonspecific binding by decreasing surface ligand density.

Xianwen Chen1, Pauline H Tan, Yanyan Zhang, Dehua Pei.   

Abstract

On-bead screening of one-bead-one-compound (OBOC) libraries provides a powerful method for the rapid identification of active compounds against molecular or cellular targets. However, on-bead screening is susceptible to interference from nonspecific binding, which results in biased screening data and false positives. In this work, we have found that a major source of nonspecific binding is derived from the high ligand loading on the library beads, which permits a macromolecular target (e.g., a protein) to simultaneously interact with multiple ligands on the bead surface. To circumvent this problem, we have synthesized a phosphotyrosyl (pY)-containing peptide library on spatially segregated TentaGel microbeads, which feature a 10-fold reduced peptide loading on the bead surface but a normal peptide loading in the bead interior. The library was screened against a panel of 10 Src homology 2 (SH2) domains including those of Csk and Fyn kinases and adaptor protein SLAP, and the specific recognition motif(s) was successfully identified for each of the domains. In contrast, when the SH2 domains were screened against a control library that contained unaltered (high) ligand loading at the bead surface, six of them exhibited varying degrees of sequence biases, ranging from minor perturbation in the relative abundance of different sequences to the exclusive selection of false positive sequences that have no measurable affinity to the target protein. These results indicate that reduction of the ligand loading on the bead surface represents a simple, effective strategy to largely eliminate the interference from nonspecific binding, while preserving sufficient amounts of materials in the bead interior for compound identification. This finding should further expand the utility of OBOC libraries in biomedical research.

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Year:  2009        PMID: 19397369      PMCID: PMC2765537          DOI: 10.1021/cc9000168

Source DB:  PubMed          Journal:  J Comb Chem        ISSN: 1520-4766


  45 in total

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6.  SH3-SH2 domain orientation in Src kinases: NMR studies of Fyn.

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7.  Structure and specificity of the SH2 domain.

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8.  Isolation of protein ligands from large peptoid libraries.

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9.  General method for rapid synthesis of multicomponent peptide mixtures.

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10.  Determination of the binding specificity of the SH2 domains of protein tyrosine phosphatase SHP-1 through the screening of a combinatorial phosphotyrosyl peptide library.

Authors:  K D Beebe; P Wang; G Arabaci; D Pei
Journal:  Biochemistry       Date:  2000-10-31       Impact factor: 3.162

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  31 in total

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2.  Solid-Phase Synthesis of β-Amino Ketones Via DNA-Compatible Organocatalytic Mannich Reactions.

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Review 4.  Protein-Catalyzed Capture Agents.

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Journal:  Chem Rev       Date:  2019-03-06       Impact factor: 60.622

5.  Diverse levels of sequence selectivity and catalytic efficiency of protein-tyrosine phosphatases.

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6.  Inhibition of Ras-Effector Interaction by Cyclic Peptides.

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7.  Screening nonspecific interactions of peptides without background interference.

Authors:  Andrew J Keefe; Kyle B Caldwell; Ann K Nowinski; Andrew D White; Amit Thakkar; Shaoyi Jiang
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8.  Discovery of peptoid ligands for anti-aquaporin 4 antibodies.

Authors:  Bindu L Raveendra; Hao Wu; Roberto Baccala; M Muralidhar Reddy; Jessica Schilke; Jeffrey L Bennett; Argyrios N Theofilopoulos; Thomas Kodadek
Journal:  Chem Biol       Date:  2013-03-21

9.  Cell-permeable bicyclic peptidyl inhibitors against T-cell protein tyrosine phosphatase from a combinatorial library.

Authors:  Hui Liao; Dehua Pei
Journal:  Org Biomol Chem       Date:  2017-11-22       Impact factor: 3.876

10.  Screening bicyclic peptide libraries for protein-protein interaction inhibitors: discovery of a tumor necrosis factor-α antagonist.

Authors:  Wenlong Lian; Punit Upadhyaya; Curran A Rhodes; Yusen Liu; Dehua Pei
Journal:  J Am Chem Soc       Date:  2013-08-01       Impact factor: 15.419

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