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HomeWebinarsSolutions for "Undruggable" Protein Targets

Solutions for "Undruggable" Protein Targets



WEBINAR

This webinar will specifically highlight high-throughput, affinity-based screening with DNA-encoded libraries, elucidation of weak or reversible small molecule–protein interactions with covalent labeling, and targeted protein degradation with bifunctional degraders. Together, these tools are accelerating the identification and development of molecules that bind and functionally alter undruggable proteins.

Who Should Attend?

  • Academic researchers
  • Pharma researchers
  • Drug discovery scientists

Speakers

John Fetter Ph.D

John Fetter Ph.D

Merck

Product Manager, Emerging Chemical Synthesis

John received his Ph.D. in biochemistry from Michigan State University where he studied cytochrome c oxidase with Shelagh Ferguson-Miller. Then he worked in drug discovery research at North Carolina State, SmithKline Beecham, and Taxolog. After that, he moved to Sigma-Aldrich, now known as Merck, where he worked on developing assays for pharmaceutical screening. He is currently a product manager in the emerging chemical synthesis where he develops products that use chemical synthesis for life science applications. Much of his focus has been on developing a portfolio of bioconjugation products. He has recently been working on making DNA-encoded libraries more accessible through their availability as off-the-shelf kits.

Angelo Lanzilotto

Angelo Lanzilotto

Merck

Technology Manager Chemistry Innovation

Angelo Lanzilotto obtained his PhD in Chemistry from the University of Basel in 2017 and has since then worked in therapeutic discovery of biologics and medicinal chemistry. He joined Merck in 2021 as a Scientific Specialist for Chemistry and later moved to the Technology Management team, where he focuses on the introduction of new products, from reagents to instrumentation, including software and services.

Webinar Information

Chemistry and synthesis

  • Protein degradation
  • Durée:1h

  • Langue:English


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