2025 ARCHIVES

Cambridge Healthtech Institute’s 7th Annual

Degraders & Molecular Glues – Part 2

Part 2: New Targets, Ligases, Assays for Induced Proximity and Degradation

September 24 - 25, 2025 ALL TIMES EDT

Hetero bifunctional molecules like proteolysis-targeting chimeras (PROTACs), monovalent molecules like molecular glues, and other novel conjugates and modalities are utilizing the ubiquitin-proteasome, lysosome, and autophagy systems to seek out previously “undruggable” targets for therapeutic intervention. Cambridge Healthtech Institute’s two-part conference on Degraders and Molecular Glues brings together experts from industry and academia to discuss both induced proximity and targeted protein degradation as viable therapeutic approaches. Part 2 focuses on emerging assays and screening strategies for identifying new drug targets, ligases, and neosubstrates for induced proximity and targeted degradation.

Wednesday, September 24

10:50 am

Welcome Remarks from Tanuja Koppal, PhD, Discovery on Target Team Lead

Tanuja Koppal, PhD, Senior Conference Director, Cambridge Healthtech Institute

11:05 am PLENARY KEYNOTE:

GLP-1 Unveiled: Key Takeaways for Next-Generation Drug Discovery

Lotte Bjerre Knudsen, PhD, Chief Scientific Advisor, Head of IDEA (Innovation&Data Experimentation Advancement), Novo Nordisk AS

This talk will explore the evolution of GLP-1 as a significant component in diabetes and obesity treatment, as well as its direct impact on multiple co-morbidities. It will highlight the role of industry innovation and scientific persistence in overcoming challenges posed by its short half-life, ultimately leading to the successful development of GLP-1 therapies. Key lessons from this journey will inform future drug discovery strategies, emphasizing that today’s drug discovery must be based on human data.

11:40 am PLENARY KEYNOTE:

Medicines, Integrins, and Organoids

Timothy A. Springer, PhD, Professor, Biological Chemistry and Molecular Pharmacology, Harvard Medical School; Senior Investigator, Boston Children's Hospital; Founder, Institute for Protein Innovation

Integrins are therapeutically important cell surface adhesion molecules that localize cells within tissues and provide many signals. Despite their essential role in stimulating growth of stem cells into organoids, the potential of integrins to regulate formation of more tissue-like organoids is unexplored. I will discuss the effects of integrin agonists and antagonists on organoid formation with a long-term goal of guiding development of vascularized, mixed-lineage organoids.

12:15 pmNetworking Lunch in the Exhibit Hall with Poster Viewing

1:45 pmWelcome Remarks

1:50 pm

Chairperson's Remarks

Abbie Macmillan-Jones, Associate Principal Scientist, Discovery Sciences, AstraZeneca

1:55 pm

FEATURED PRESENTATION: Advances in the Systematic Discovery of Molecular Glue Degraders

Eric Fischer, PhD, Associate Professor, Biological Chemistry and Molecular Pharmacology, Harvard Medical School; Director Center for Protein Degradation, Dana-Farber Cancer Institute

In recent years, the co-opting of ubiquitin ligases by small molecules for the targeted protein degradation of disease-causing proteins has emerged as a powerful pharmacologic modality. While the discovery of PROTACs has become a mainstay of drug discovery, discovery of novel molecular glues beyond CRBN modulators remains a major challenge for the field. I will present recent work on understanding the principles that govern molecular glue interactions, updates on our discovery platforms and recent examples of success to expand the repertoire of ligases enabled for molecular glues.

2:55 pm

Discovering Novel CRBN Molecular Glue Degraders through Integrated Generative AI and Lab Chemistry Capabilities

HongBo Zhang, VP, HitChem

Cereblon (CRBN)-based molecular glues have emerged as a transformative approach in drug discovery. However, the discovery of novel CRBN molecular glue degraders remains a significant challenge.

HitChem has developed an AI-driven molecular generation platform to support the glue discovery. Leveraging this model and a set of validated CRBN binders, we constructed a focused virtual library of over 100 million molecules. From this space, we further curated 57,000 structurally diverse compounds prioritized by scaffold diversity and CRBN structural modeling as our physical library.

High-throughput screening using the library has successfully identified novel CRBN molecular glues against VAV1, NEK7, CDK2, STAT6 with significant higher hit rate compared to commercial libraries. And the identified hit series exhibit comparable degradation profiles and selectivity but with larger IP space.

3:25 pmRefreshment Break in the Exhibit Hall with Poster Viewing

Recharge during our refreshment break! Visit booths, view posters, connect with peers, and turn in your Game Cards for a chance to win a raffle prize. Don’t miss the opportunity to meet the Venture Capitalists who will be participating in the panel following the break. And Connect the DOT’s with participants driving the Collaborations Discussion following the VC panel.

4:15 pm

PLENARY PANEL DISCUSSION: Venture Capitalist Insights into Trends in Drug Discovery

PANEL MODERATOR:

Daniel A. Erlanson, PhD, Chief Innovation Officer, Frontier Medicines Corporation

Topics to be discussed:

Key drivers of innovation in drug discovery
Overcoming hurdles in translating discoveries from the lab to the clinic
Impact of AI/machine learning, emerging drug modalities, pursuit of challenging drug targets
Navigating the current regulatory and funding environment
Perspectives on upcoming challenges and opportunities in drug development

PANELISTS:

Olga Danilchanka, PhD, Partner, MRL Ventures Fund

Chris De Savi, PhD, CSO Partner, Curie Bio

Jamie Kasuboski, PhD, Partner, Luma Group

Brendan Kelly, PhD, Principal, Lightstone Ventures

David Kolesky, PhD, Principal, MPM Capital LLC

Blair Willette, PhD, Associate, KdT Ventures

5:15 pmDinner Short Course Registration*

IN-PERSON PLENARY DISCUSSION: Connecting the DOTs to Spark Change!

Shruthi Bharadwaj, PhD, Pharma Leader & Executive, Investor, Advisor & Start-Up Partner

Sean Ekins, PhD, Founder & CEO, Collaborations Pharmaceuticals, Inc.

Saudat Fadeyi, PhD, MBA, Head, Business Development & Strategy, Samyang Biopharm USA, Inc.

Raquel Mura, PharmD, Founder, RGM Life Sciences Consulting; Former Vice President & Head, R&D North America, Sanofi

Nisha Perez, ScD, MS, MSPM, Head of DMPK & Clinical Pharmacology, HotSpot Therapeutics

Join us for an hour of inspiring, informal discussions on how to forge connections and create impactful ecosystems that will help you think, act, and thrive. We have invited pharma, biotech, and academic leaders to share their stories and experiences and to discuss key learnings. There will be time for open discussion and networking.

This session will not be recorded for on-demand viewing. See details on our Plenary Sessions Page.

6:00 pmDinner Short Courses*

*All Access Package or separate registration required. See Short Courses page for details.

8:30 pmClose of Day

Thursday, September 25

7:30 amRegistration Open and Morning Coffee

8:45 am

Chairperson's Remarks

Charles Wartchow, PhD, Associate Director, Discovery Sciences, Novartis Institutes for BioMedical Research

8:50 am

FEATURED PRESENTATION: Attenuating Oncogenic Transcription with Small Molecules

Angela Koehler, PhD, Professor, Biological Engineering, Massachusetts Institute of Technology

The lecture reviews recent advances in the lab involving successful targeting strategies, including discussion of compounds that modulate MYC-driven transcription via mechanisms involving the MAX partner protein or the transcriptional kinase CDK9. Additionally, new and unpublished work related to targeting fusion oncoproteins arising in pediatric cancers such as alveolar rhabdomysosarcoma will be discussed.

9:35 am

Targeting MYC and Oncogenic p53 through LZK Inhibition or Degradation to Treat Head and Neck Cancers

John Brognard, PhD, Professor of Surgery, Upstate Medical University

We determined that LZK (encoded by MAP3K13) is a therapeutic target in HNSCC and showed that inhibition with small molecule inhibitors decreases the viability of HNSCC cells with amplified MAP3K13. A drug-resistant mutant of LZK blocks decreases in cell viability due to LZK inhibition, indicating on-target activity by two separate small molecules. Inhibition of LZK catalytic activity suppressed tumor growth in HNSCC PDX models with amplified MAP3K13. We designed proteolysis-targeting chimeras (PROTACs) and demonstrate that our lead PROTAC promotes LZK degradation and suppresses expression of GOF p53 and c-MYC, leading to impaired viability of HNSCC.

10:05 amIn-Person Breakouts

In-Person Breakouts are informal, moderated discussions, allowing participants to exchange ideas and experiences and develop future collaborations around a focused topic. Each discussion will be led by a facilitator, or facilitators, who keeps the discussion on track and the group engaged. To get the most out of this format, please come prepared to share examples from your work, be a part of a collective, problem-solving session, and participate in active idea sharing. Please visit the Breakouts page on the conference website for a complete listing of topics and descriptions.

In-Person Only BREAKOUT 1: Pursuing Novel Degradation Modalities, E3 Ligases for Challenging Drug Targets

Mikolaj Slabicki, PhD, Assistant Professor, MGH/Broad Institute

Charles Wartchow, PhD, Associate Director, Discovery Sciences, Novartis Institutes for BioMedical Research

In-Person Only BREAKOUT 2: Screening and Optimization of Degraders & Glues

Abbie Macmillan-Jones, Associate Principal Scientist, Discovery Sciences, AstraZeneca

Milad Rouhimoghadam, PhD, Senior Scientist I, Small Molecule Therapeutics & Platform Technology, AbbVie

10:50 amCoffee Break in the Exhibit Hall with Book Raffle, Best of Show Poster and Exhibitor Awards Announced

Meet new collaborators, and network with clients, colleagues, and exhibitors. Make your vote count for the People’s Choice Best of Show Exhibitor award and plan to stay and cheer the winner! Remember to enter your name for the Book Raffle!

11:30 am

Delivering on Cascades for Next-Generation Degraders: Translating Innovation into Impact

Abbie Macmillan-Jones, Associate Principal Scientist, Discovery Sciences, AstraZeneca

Following the success of PROTACs laying the framework for modulation of protein levels as a therapeutic strategy, the field of protein degradation has witnessed an unprecedented expansion in new drug modalities. This talk will discuss strategies to discover and develop these next generation molecules, translating basic research innovation into therapeutically active compounds.

12:00 pm

Physicochemical Guides for the Design of Orally Bioavailable PROTAC Protein Degraders

Erika Vieira Araujo, PhD, Principal Research Investigator, Discovery Chemistry, Arvinas Inc.

Through a retrospective analysis of the pharmacokinetic profiles of a large set of PROTAC molecules, we have derived PROTAC design constraints on physicochemical properties associated with higher probability of oral bioavailability. This data was further used to train a machine-learning model to predict oral-absorption performance to further prospective design efforts of orally bioavailable molecules.

12:30 pmEnjoy Lunch on Your Own

1:35 pmDessert Break in the Exhibit Hall with Book Raffle, Best of Show Poster Award, and Last Chance for Poster Viewing

Enjoy dessert and coffee during our final exhibit hall break. Did you connect with all the service providers and poster presenters? You never know what you missed! Stay till the end to maximize your time in the exhibit hall and to celebrate our Best of Show Poster award winner!

2:15 pm

Chairperson's Remarks

Gisele Nishiguchi, PhD, Group Leader, St. Jude Children's Research Hospital

2:20 pm

Multimodal Screening Strategies to Identify Novel Cereblon Neosubstrates

Gisele Nishiguchi, PhD, Group Leader, St. Jude Children's Research Hospital

The design of molecular glue degraders (MGD) has been challenging and the discovery of novel MGD/neosubstrate pairs has relied primarily on different screening strategies. In this talk, I will discuss our multipronged screening approaches (phenotypic, targeted, and proteome-wide) against a molecular glue library based on cereblon binders and the discovery of novel degrader-neosubstrate pairs.

2:50 pm

NanoBRET-Powered High-Throughput Platform for the Discovery of Molecular Glues

Milad Rouhimoghadam, PhD, Senior Scientist I, Small Molecule Therapeutics & Platform Technology, AbbVie

We introduce a NanoBRET-powered high-throughput platform that lights up molecular glue activity in live cells. By capturing real-time E3 ligase–substrate interactions, this assay enables rapid, scalable discovery of glue degraders with high sensitivity and physiological relevance, offering a powerful tool to unlock new therapeutic mechanisms and expand the degradable proteome.

3:20 pm

Expanding the Set of Zinc Finger Proteins Accessible to Drug-Induced Protein Degradation by CRBN

Mikolaj Slabicki, PhD, Assistant Professor, MGH/Broad Institute

The Slabicki Laboratory investigates the mechanistic basis of protein degradation by leveraging functional genomics and reprogramming the ubiquitin-proteasome system. Using advanced screening and biochemical approaches, we elucidate target-ligase interactions to accelerate therapeutic discovery for diseases lacking effective treatments. In our current work, we characterize neosubstrate recognition by CRBN, revealing how auxiliary degron interactions define and expand target scope and selectivity, enabling the rational design of more selective protein degraders.

3:50 pm

A Highly Productive Platform for Discovery of Targeted Protein Degraders

Shigeru Furukubo, PhD, Vice President, Chemistry, FIMECS Inc.

Our proprietary platform, RaPPIDS, facilitates the rapid production of degrader molecules and effective evaluation of targeted protein degradation. The high productivity of this platform enables us to discover not only novel E3 ligase binders by taking phenotypic-first approach but also well-optimized degraders with suitable DMPK profile. In this talk, I will share some case studies from our ongoing research programs.

4:20 pmClose of Conference