2025 ARCHIVES

Cambridge Healthtech Institute's 15th Annual

Driving Clinical Success in Antibody-Drug Conjugates

Designing the Magic Bullet

May 15 - 16, 2025 ALL TIMES EDT

As of 2024, 15 ADC drugs have been approved globally, with over 100 others in clinical development—underscoring the ongoing excitement and innovation surrounding ADCs in cancer therapy. Once primarily used in late-stage treatment for specific blood cancers, ADCs are now advancing toward broader applications, including solid tumors and earlier lines of treatment. The Driving Clinical Success in Antibody-Drug Conjugates conference will delve into the future of ADC development, focusing on novel payloads and mechanisms of action (MOAs), engineering strategies to enhance the therapeutic window, and opportunities to expand indications and explore combination therapies.

Sunday, May 11

1:00 pmMain Conference Registration

2:00 pmRecommended Pre-Conference Short Course

SC2: Safety & Efficacy of Bispecifics and ADCs

*Separate registration required. See short course page for details.

Thursday, May 15

7:45 amRegistration and Morning Coffee

8:25 am

Chairperson's Remarks

Greg M. Thurber, PhD, Associate Professor, Chemical Engineering & Biomedical Engineering, University of Michigan

8:30 am

Degrader-Antibody Conjugates (DACs) Unlock Heterobifunctional Degraders through mAb-Like Pharmacokinetics and Excellent in vivo Efficacy

Jonas Helma-Smets, PhD, Founder & CSO, Tubulis GmbH

New ADC payload strategies are needed to address emerging drug resistance and limited treatment durability. Degrader-Antibody Conjugates (DACs) could significantly expand the number of druggable payload targets; however, conjugation and identification of suitable degraders remain challenging. Here, we report a new DAC platform ensuring excellent DAC stability antibody-mediated delivery of functional degraders enabling long-lasting responses even after single-dose injections in preclinical animal models.

9:00 am

The Design and Optimization of Degrader-Antibody Conjugates

Stephanie M. Monson, PhD, Principal Scientist & Group Leader, Conjugation & Chemical Biology, Genentech Inc.

Degrader Antibody Conjugates (DACs) represent a novel therapeutic approach that combines the specificity of antibodies with the potency of protein degraders. The design and optimization of DACs involve careful consideration of factors such as antibody selection, linker chemistry, and TPD potency. By precisely engineering these components, researchers aim to create highly effective and selective DACs for the treatment of various diseases, including cancer.

9:30 am

PROxAb Shuttle: A Plug & Play Solution for Targeted Antibody-Mediated Degrader Delivery

Hendrik Schneider, PhD, Principal Scientist, Merck KGaA, Darmstadt, Germany

Targeted protein degradation has emerged as a promising therapeutic strategy for addressing challenging molecular pathologies. However, achieving tissue selectivity remains challenging. The PROxAb Shuttle approach introduces a non-covalent platform for antibody-mediated targeted delivery of degraders. By enhancing pharmacokinetics and prolonging degrader half-lives from hours to days, this system aims to improve the selectivity and efficacy of tumor-targeting therapies, facilitating significant anti-tumor responses in vivo.

10:00 am

VBC106: A First-in-class FOLR1/MSLN Targeted Tri-specific Antibody Drug Conjugate (ADC) in Ovarian Cancer, Endometrial Cancer, Lung Adenocarcinoma and Beyond

Jing Li, PhD, CEO, VelaVigo

10:30 amCoffee Break in the Exhibit Hall with Poster Viewing

11:15 amTransition to Plenary Fireside Chat

11:25 am

Riding the Next Biotech Wave—Trends in Biotech Investments, Partnering, and M&As

PANEL MODERATOR:

Jakob Dupont, MD, Executive Partner, Sofinnova Investments

Emerging Biotherapeutic Modalities, Technologies and Innovations— ADCs, radiopharmaceuticals, GLP-1, AI, machine learning, and other exciting trends to watch
Introduction to different strategies for investments, M&As, partnering, licensing etc.
Investing in platforms versus assets
Advice on funding options for start-ups, early to late stage clinical programs, etc.

PANELISTS:

Hong Xin, PhD, Senior Director, External Innovation Search & Evaluation, Johnson & Johnson

Shyam Masrani, Partner, Medicxi

Uciane Scarlett, PhD, Former Principal, MPM BioImpact

Anthony B. Barry, PhD, Executive Director, ES&I Lead, Biotherapeutics, Technologies, and Digital, Pfizer Inc.

12:25 pmLuncheon in the Exhibit Hall and Last Chance for Poster Viewing

1:55 pm

Chairperson's Remarks

John M. Lambert, PhD, Consultant

2:00 pm

Reviewing the Development of DXd ADC Technology & the Latest Clinical Results

Akiko Zembutsu, PhD, Head of Group I, Discovery Research Laboratories I, R&D Division, Daiichi Sankyo Co., Ltd.

Trastuzumab deruxtecan, utilizing DXd ADC technology, is transforming HER2 treatment by demonstrating strong efficacy not only in HER2-high, but also in HER2 ultra-low cases. Daiichi Sankyo is applying this DXd ADC technology to various targeted antibodies and advancing clinical trials. In my presentation, I will introduce the unique features of the technology and present the latest nonclinical and clinical data.

2:30 pm

Development of Glucocorticoid Receptor Modulator ADC for Inflammatory Diseases

Michael McPherson, PhD, Research Fellow, Antibody Drug Conjugates, Technology and Therapeutic Platforms, AbbVie

Glucocorticoids (GCs) are potent anti-inflammatory drugs, but their widespread use is limited by systemic side effects. To address this, we have developed Glucocorticoid Receptor Modulator (GRM) Antibody-Drug Conjugates (ADCs) for inflammatory diseases. By precisely targeting the drug, ADCs aim to minimize systemic exposure and reduce adverse effects, while maximizing therapeutic efficacy. This innovative approach holds significant promise for treating a variety of inflammatory conditions, including autoimmune diseases and allergic disorders.

3:00 pm PANEL DISCUSSION:

Clinical Performance Evaluation of TOPO1 ADCs

PANEL MODERATOR:

Rakesh Dixit, PhD, DABT, CEO & President, Bionavigen Oncology, LLC and CSO, TMAB Therapeutics, Regio Biosciences

Why TOPO1 ADCs are not succeeding in lung cancer
What's next in the horizon for TOPO1 ADCs?

PANELISTS:

Hanspeter Gerber, PhD, CSO, Sutro Biosciences

Robert J. Lutz, PhD, CSO, Iksuda Therapeutics

Gilles JA Gallant, PhD, Chief Development Officer, Mythic Therapeutics

4:00 pmNetworking Refreshment Break

4:30 pm

A Novel Antibody (Oligo)-Drug Conjugate to Treat Cancer

David M. Evans, PhD, Head of Discovery, Research, Sirnaomics Inc.

We have designed a novel siRNA containing gemcitabine in its backbone. This has demonstrated potent activity in preclinical models of pancreatic cancer, NSCLC and TNBC. This talk will demonstrate the synthesis and activity when conjugated to cetuximab for delivery to tumors in vitro and in vivo.

5:00 pm

FORCE^TMPlatform Delivers Functional Improvement in Neuromuscular Disorders

Cody Desjardins, PhD, Director, Neuromuscular Research, Dyne Therapeutics Inc.

FORCE is a modular platform which enables delivery of chemically diverse therapeutic payloads with widespread distribution to muscle and CNS. The FORCE platform is translating into the clinic with the ACHIEVE and DELIVER trials for DM1 and DMD, respectively. These encouraging clinical data and strong preclinical efficacy in FSHD and Pompe disease models support the potential of FORCE to address neuromuscular disorders with high unmet medical needs.

5:30 pmClose of Day

Friday, May 16

7:15 amRegistration Open

7:30 amInteractive Discussions

Interactive Discussions 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 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 Interactive Discussions page on the conference website for a complete listing of topics and descriptions.

TABLE 2: Opportunities for Protein Engineering in ADC Development

Greg M. Thurber, PhD, Associate Professor, Chemical Engineering & Biomedical Engineering, University of Michigan

8:25 am

Chairperson's Remarks

Robert J. Lutz, PhD, CSO, Iksuda Therapeutics

8:30 am KEYNOTE PRESENTATION:

Protein Engineering Strategies to Improve the Efficacy of Antibody-Drug Conjugates

Greg M. Thurber, PhD, Associate Professor, Chemical Engineering & Biomedical Engineering, University of Michigan

Antibody-drug conjugates are showing tremendous promise in the clinic with multiple FDA approvals and clinical-state compounds. A significant effort has improved the linker, payload, and conjugation strategies, but less emphasis has been placed on engineering the protein. In this talk, we will present strategies for antibody engineering including the use of multivalent and/or biparatopic antibodies, epitope selection with antibody/ADC combinations, and Fc-engineering to improve the therapeutic window.

9:00 am

Reversible Chemical Modification of Antibodies: Modulating FcγR Binding to Maintain Anti-Tumor Activity and Mitigate Systemic Immune Activation

Philip N. Moquist, PhD, Associate Research Fellow, Chemistry, Pfizer Oncology

Here we present a method for tuning effector function inspired by antibody-drug conjugates. This methodology uses conjugation of polyethylene glycol (PEG) to native cysteines of an antibody to impair FcgR binding. Attenuated effector function can be permanent or restored through a de-conjugation process. Impacts of reversible PEGylation were assessed and applied to an agonist CD40 antibody. The PEGylated constructs displayed significant reductions in systemic cytokine production in vivo, while retaining efficacy.

9:30 am

Exploring the Design of Selectively-Targeted Payloads with Quantitative Systems Pharmacology

Eshita Khera, PhD, Principal Scientist II, Modeling & Simulation & PK Sciences, Novartis BioMedical Research

Over 90% of clinical ADCs use pan-cytotoxic payloads, but there is emerging interest in selectively-targeted payloads such as protein inhibitors and degraders. However, designing ADCs with non-traditional payloads is even more complex than cytotoxic ADCs, and challenging to optimize empirically. The proposed talk will highlight some new guiding principles for designing non-traditional ADCs, guided by vignettes of integrated lab-to-model workflows powered by Quantitative Systems Pharmacology.

10:00 am

Enhancing ADCs Both within and outside the Tumor with Sutro’s Platform Technologies Leads to a Higher Therapeutic Index

Hanspeter Gerber, PhD, CSO, Sutro Biosciences

The recent renaissance of ADCs was enabled by the dramatic increase in their therapeutic indexes, which can be achieved in two ways: either by making ADCs safer outside the tumors, resulting in an increased maximum tolerated dose—or inside the tumor, by improving their potency or reducing resistance formation. I will discuss several examples of how we achieved this goal with our next-generation Topo1 ADC platform.

10:30 amNetworking Coffee Break

11:00 am

Bicycle Drug Conjugates - Lessons from the Clinic

Liuhong Chen, PhD, Vice President, Platform Innovation, Bicycle Therapeutics

Bicycle Therapeutics is developing a unique class of chemically synthesized bicyclic peptide (Bicycle) medicines, including its Bicycle Drug Conjugates (BDCs) currently in clinical development for the treatment of solid tumors. Bicycle molecules are constrained peptides characterized by high affinity and selectivity, small size enabling fast tissue penetration, modularity for conjugation and favorable pharmacokinetics. These advantages will be discussed in the context of preclinical data and the emerging clinical picture.

11:30 am

ADC Designs with Tumor-Selective Linkers and Novel ProAlk Payload for Differentiated Tolerability Profiles

Jutta Deckert, PhD, Vice President, Research & Development, Iksuda Therapeutics

This presentation aims to 1) highlight stable bioconjugation approaches for increased ADC stability in vitro and in vivo, 2) describe tumor-selective linker designs that are aimed to improve the therapeutic index of ADCs by altering the toxicity profile and increasing tolerability, and 3) introduce ProAlk as a novel ADC payload with a differentiated mechanism of action and provide preclinical proof-of-concept studies.

12:00 pm

Novel mavg-MMAU Linker-Payload Improves Both Efficacy and Tolerability of Auristatin ADCs Topo 1i and Dual-Payload ADCs with Hydrophilic Glycopeptide Linker

Juhani Saarinen, CEO, Glykos Finland Oy

Auristatin glycoside ADCs with stabilized glycopeptide linker provide exceptionally wide therapeutic window and improved potency. Preclinical validation of CD33, TYRP-1, and HER2 targeting MMAU ADCs.
Next-generation auristatin ADCs were developed based on MMAU (glucuronylated prodrug of MMAE) enabling both DAR=4 and DAR=8 ADCs with high potency.
The novel mavg-MMAU linker-payloads enabled simultaneous improvements in both in vivo efficacy and tolerability; bystander efficacy and resistance to MDR drug efflux; and improved PK and lower off-target toxicity compared to vedotin ADCs.
The improved linker was further applied to novel exatecan linker-payloads and dual payload ADCs.

12:30 pmClose of Summit