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Dive into the research topics where Scott F. Singleton is active.

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Featured researches published by Scott F. Singleton.


Journal of Biomolecular Screening | 2009

Inhibitors of RecA Activity Discovered by High-Throughput Screening: Cell-Permeable Small Molecules Attenuate the SOS Response in Escherichia coli

Tim J. Wigle; Jonathan Z. Sexton; Anna V. Gromova; Mallinath B. Hadimani; Mark A. Hughes; Ginger R. Smith; Li An Yeh; Scott F. Singleton

The phenomenon of antibiotic resistance has created a need for the development of novel antibiotic classes with nonclassical cellular targets. Unfortunately, target-based drug discovery against proteins considered essential for in vitro bacterial viability has yielded few new therapeutic classes of antibiotics. Targeting the large proportion of genes considered nonessential that have yet to be explored by high-throughput screening, for example, RecA, can complement these efforts. Recent evidence suggests that RecA-controlled processes are responsible for tolerance to antibiotic chemotherapy and are involved in pathways that ultimately lead to full-fledged antibiotic resistance. Therefore inhibitors of RecA may serve as therapeutic adjuvants in combination chemotherapy of bacterial infectious diseases. Toward the goal of validating RecA as a novel target in the chemotherapy of bacterial infections, the authors have screened 35,780 small molecules against RecA. In total, 80 small molecules were identified as primary hits and could be clustered in 6 distinct chemotype clades. The most potent class of hits was further examined, and 1 member compound was found to inhibit RecA-mediated strand exchange and prevent ciprofloxacin-induced SOS expression in Escherichia coli. This compound represents the first small molecule demonstrating an ability to inhibit the bacterial SOS response in live bacterial cell cultures. (Journal of Biomolecular Screening 2009:1092-1101)


Current Chemical Genomics | 2010

Novel Inhibitors of E. coli RecA ATPase Activity

Jonathan Z. Sexton; Tim J. Wigle; Qingping He; Mark A. Hughes; Ginger R. Smith; Scott F. Singleton; Alfred L. Williams; Li An Yeh

The bacterial RecA protein has been implicated as a bacterial drug target not as an antimicrobial target, but as an adjuvant target with the potential to suppress the mechanism by which bacteria gain drug resistance. In order to identify small molecules that inhibit RecA/ssDNA nucleoprotein filament formation, we have adapted the phosphomolybdate-blue ATPase assay for high throughput screening to determine RecA ATPase activity against a library of 33,600 compounds, which is a selected representation of diverse structure of 350,000. Four distinct chemotypes were represented among the 40 validated hits. SAR and further chemical synthesis is underway to optimize this set of inhibitors to be used as antimicrobial adjuvant agents.


Journal of the American Chemical Society | 2011

Direct Detection of Structurally Resolved Dynamics in a Multiconformation Receptor−Ligand Complex

Mary J. Carroll; Anna V. Gromova; Keith R. Miller; Hao Tang; Xiang Simon Wang; Ashutosh Tripathy; Scott F. Singleton; Edward J. Collins; Andrew L. Lee

Structure-based drug design relies on static protein structures despite significant evidence for the need to include protein dynamics as a serious consideration. In practice, dynamic motions are neglected because they are not understood well enough to model, a situation resulting from a lack of explicit experimental examples of dynamic receptor-ligand complexes. Here, we report high-resolution details of pronounced ~1 ms time scale motions of a receptor-small molecule complex using a combination of NMR and X-ray crystallography. Large conformational dynamics in Escherichia coli dihydrofolate reductase are driven by internal switching motions of the drug-like, nanomolar-affinity inhibitor. Carr-Purcell-Meiboom-Gill relaxation dispersion experiments and NOEs revealed the crystal structure to contain critical elements of the high energy protein-ligand conformation. The availability of accurate, structurally resolved dynamics in a protein-ligand complex should serve as a valuable benchmark for modeling dynamics in other receptor-ligand complexes and prediction of binding affinities.


Biochemistry | 1992

Influence of pH on the equilibrium association constants for oligodeoxyribonucleotide-directed triple helix formation at single DNA sites

Scott F. Singleton; Peter B. Dervan


Biochemistry | 1993

Equilibrium association constants for oligonucleotide-directed triple helix formation at single DNA sites: linkage to cation valence and concentration

Scott F. Singleton; Peter B. Dervan


Journal of the American Chemical Society | 1992

Thermodynamics of oligodeoxyribonucleotide-directed triple helix formation: an analysis using quantitative affinity cleavage titration

Scott F. Singleton; Peter B. Dervan


Journal of the American Chemical Society | 1994

Temperature Dependence of the Energetics of Oligonucleotide-Directed Triple-Helix Formation at a Single DNA Site

Scott F. Singleton; Peter B. Dervan


Biochemistry | 2006

Conformationally selective binding of nucleotide analogues to Escherichia coli RecA: a ligand-based analysis of the RecA ATP binding site.

Tim J. Wigle; and Andrew M. Lee; Scott F. Singleton


Journal of the American Chemical Society | 2003

Direct Evaluation of a Mechanism for Activation of the RecA Nucleoprotein Filament

Alberto I. Roca; Scott F. Singleton


Biochemistry | 2006

Intersubunit electrostatic complementarity in the RecA nucleoprotein filament regulates nucleotide substrate specificity and conformational activation

Andrew M. Lee; Scott F. Singleton

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Peter B. Dervan

California Institute of Technology

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Tim J. Wigle

University of North Carolina at Chapel Hill

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Ginger R. Smith

North Carolina Central University

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Jonathan Z. Sexton

North Carolina Central University

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Mark A. Hughes

North Carolina Central University

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Alfred L. Williams

North Carolina Central University

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Anna V. Gromova

University of North Carolina at Chapel Hill

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Li An Yeh

North Carolina Central University

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Qingping He

North Carolina Central University

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