Bi-weekly: Thursdays, 12 pm EDT/EST, 9 am PT/PST, 5 pm BST/BDT, 6 pm CEST/CET
https://dfci.zoom.us/webinar/register/WN_m7JJaw52T8yZYt8-ykL6UQ
Some seminars were recorded and accessible for a limited time on our youtube channel.
Upcoming Speakers

April 17th, 2025
Host: Shourya S Roy Burman / Mikolaj Slabicki
Charlotte Crowe
University of Dundee
Mechanisms of degrader-targeted protein ubiquitinability
Dr Charlotte Crowe is a postdoctoral researcher in Alessio Ciulli’s laboratory at the Centre for Targeted Protein Degradation (CeTPD) at the University of Dundee. She is originally from Strasbourg, France. She moved to Scotland in 2015 to study an MChem in Chemistry at the University of St Andrews, graduating with Honours in 2020. Her PhD, focusing on using chemical, structural and biophysical approaches to understand the mechanism of action of small molecule degraders in Targeted Protein Degradation (TPD), with a particular focus on Cullin RING E3 ligases, was supervised by Professor Alessio Ciulli and Professor Ron Hay at the University of Dundee, and Dr Hannah Maple from Tocris, Bio-Techne. In 2024, she joined the Ciulli lab as a postdoctoral researcher, and from January 2025 she has been working in the CeTPD LITE project team with the Michael J. Fox Foundation developing degraders to tackle Parkinson’s disease.

Alessandra Salerno
University of Dundee
FerroTACs: harnessing ferrocene as a molecular hinge for the design of conformationally dynamic PROTAC linkers.
Alessandra Salerno has been a postdoctoral research fellow at the Centre for Targeted Protein Degradation at the University of Dundee since 2023, working under the supervision of Professor Alessio Ciulli. She earned her PhD in Medicinal Chemistry from the University of Bologna (Italy) in 2022, enriching her academic background through various international research experiences. Currently funded by a Marie Skłodowska-Curie Fellowship through UKRI, her research focuses on the development of innovative chemical modalities in the field of PROTACs and targeted protein degradation (TPD). Her recent work includes the design of novel PROTAC linkers incorporating unique chemotypes (i.e., FerroTACs) and the application of combinatorial chemistry strategies to streamline PROTAC identification. Her wider scientific interests span proximity labelling methods for probing protein-protein interactions, as well as the discovery of anti-infective agents.

May 1st, 2025
Host: Hubert Huang
Larry Hamann
Interdict Bio
Sequence-Selective Translation Inhibition as a Novel, Proximity-Based Cancer Therapeutic Modality
Larry Hamann is currently co-founder, president and CEO of Interdict Bio, pioneering small-molecule context-dependent translation inhibitors for addressing historically undruggable targets in oncology and neurodegeneration. Previously, he was Global Head of Discovery at Takeda. Prior to Takeda, he was Corporate VP and Global Head of Small Molecule Drug Discovery at Celgene, and prior to Celgene, stints at Novartis, Bristol-Myers Squibb and Ligand. In >30 years in drug discovery, his teams have advanced >22 molecules into the clinic, including ONGLYZA™, DAKLINZA™, and branaplam, as well as mezigdomide, golcadomide, and gridegalutamide - targeted protein degraders all currently in Phase III. He is co-inventor on >70 patents, co-author on >90 scientific publications, and advises many biotechs and VCs. He is a recipient of the ACS Heroes of Chemistry Award, the ACS Division of Medicinal Chemistry Award, and was inducted into the Medicinal Chemistry Hall of Fame. Larry holds a Ph.D. in organic chemistry from the University of Michigan.

Nick Till
Stanford University
Redirecting Trogocytosis for Targeted Protein Transfer
Nick Till earned a B.A. in Chemistry from Reed College where he studied bismuth catalysis in Professor Rebecca LaLonde’s lab. After internship experiences at Gilead and Genentech, Nick joined Professor David W. C. MacMillan’s lab at Princeton University where he completed his Ph.D. in Chemistry. There he developed new Ni/photoredox dual catalytic reactions and elucidated elementary mechanistic steps relevant to cross-coupling reactions that are widely employed in academic and industrial settings. He then joined Professor Carolyn Bertozzi’s lab at Stanford University where he works as an NIH Postdoctoral Fellow using chemical approaches to manipulate the cell surface through various induced proximity modalities.

May 15th, 2025
Host: Katherine Donovan
Rebecca Metivier
DFCI
Unveiling the hidden interactome of CRBN molecular glues with chemoproteomics.
Rebecca received her BS in Marine Biology from Roger Williams University and her MS in Chemical Biology from Boston College. After receiving her Masters, Rebecca worked as a Research associate in the proteomics group in the Center for Protein degradation where she focused on target identification using established methodology as well as leading the development of new workflows within the group. Rebecca joined the the TPD Proteomics Core as a Scientist in 2021 where she employs various chemoproteomics methods to study cellular responses to protein degraders and molecular glues. She also leads the development and optimization of new methods and technologies for the group.

Martin Steger
NEOsphere Biotechnologies
Integrated high-throughput proteomics platform for degrader target discovery and validation.
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PhD in molecular cancer research from the University of Zurich (Switzerland)
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Postdoc at the MPI of Biochemistry in Martinsried (Germany), working on Parkinson's disease and using global proteomics and phosphoproteomics to discover the first molecular marker for LRRK2 protein kinase
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Currently industry researcher (Head of Degrader Biochemistry and Co-founder) at NEOsphere Biotechnologies, using state-of-the-art proteomics methods for screening protein degraders and validating target candidates of degraders.
May 29th, 2025
Host: Zuzanna Kozicka
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