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Thomas Kodadek

Thomas Kodadek

· Professor of Chemistry

University of Florida · Medicinal Chemistry

Active 1983–2024

h-index67
Citations15.8k
Papers33942 last 5y
Funding$73.3M
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Research topics

  • Biochemistry
  • Chemistry
  • Computer Science
  • Biology
  • Combinatorial chemistry
  • Stereochemistry
  • Genetics
  • Nanotechnology
  • Database
  • Materials science
  • Computational biology
  • Chromatography
  • Cell biology
  • Physics
  • Biophysics

Selected publications

  • Reversible Assembly of Proteolysis Targeting Chimeras

    ACS Chemical Biology · 2023 · 27 citations

    Senior authorCorresponding
    • Cell biology
    • Chemistry
    • Biology

    PROteolysis TArgeting Chimeras (PROTACs) are of significant current interest for the development of probe molecules and drug leads. However, they suffer from certain limitations. PROTACs are rule-breaking molecules with sub-optimal cellular permeability, solubility, and other drug-like properties. In particular, they exhibit an unusual dose-response curve where high concentrations of the bivalent molecule inhibit degradation activity, a phenomenon known as the hook effect. This will likely complicate their use in vivo. In this study, we explore a novel approach to create PROTACs that do not exhibit a hook effect. This is achieved by equipping the target protein and E3 ubiquitin ligase ligands with functionalities that undergo rapid and reversible covalent assembly in cellulo. We report the development of Self-Assembled Proteolysis Targeting Chimeras that mediate the degradation of the Von Hippel-Lindau E3 ubiquitin ligase and do not evince a hook effect.

  • High‐Throughput Quality Control Assay for the Solid‐Phase Synthesis of DNA‐Encoded Libraries of Macrocycles**

    Angewandte Chemie International Edition · 2021 · 24 citations

    Senior authorCorresponding
    • Computer Science
    • Combinatorial chemistry
    • Chemistry

    There is considerable interest in the development of libraries of scaffold-diverse macrocycles as a source of ligands for difficult targets, such as protein-protein interaction surfaces. A classic problem in the synthesis of high-quality macrocyclic libraries is that some linear precursors will cyclize efficiently while some will not, depending on their conformational preferences. We report here a powerful quality control method that can be employed to readily distinguish between scaffolds that do and do not cyclize efficiently during solid-phase synthesis of thioether macrocycles without the need for tedious liquid chromatography/mass spectrometry analysis. We demonstrate that this assay can be employed to identify linear impurities in a DNA-encoded library of macrocycles. We also use the method to establish a useful quality control protocol for re-synthesis of putative macrocyclic screening hits.

  • Solid-phase synthesis of DNA-encoded libraries <i>via</i> an “aldehyde explosion” strategy

    Chemical Communications · 2020 · 48 citations

    Senior authorCorresponding
    • Combinatorial chemistry
    • Chemistry
    • Biochemistry

    We report chemistry suitable for the solid-phase synthesis of DNA-encoded libraries with an unusually high level of structural diversity. The strategy involves "exploding" an immobilized aldehyde into a plethora of different functional groups under DNA-compatible conditions.

Recent grants

Frequent coauthors

  • Stephen Albert Johnston

    Phoenix (United States)

    36 shared
  • Young Ho Kim

    Korea University

    30 shared
  • Jonathan R. Pollack

    Stratford University

    30 shared
  • Lauren A. Byers

    29 shared
  • Michael Peyton

    University of Wisconsin–Madison

    29 shared
  • Yang Xie

    29 shared
  • Boning Gao

    Southeast University

    29 shared
  • David S. Shames

    Marker Gene Technologies (United States)

    29 shared

Education

  • Post-doc, Biochemistry

    University of California San Francisco

    1987
  • Ph.D., Chemistry

    Stanford University

    1985
  • BS, Chemistry and Biology

    University of Miami

    1981

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