2025 ARCHIVES
Monday, January 13
8:00 amRegistration and Morning Coffee
8:50 amOrganizer's Welcome Remarks
Nikki Cerniuk, Conference Producer, Cambridge Healthtech Institute
Chairperson's Opening Remarks
Danielle Dettling, CSO and Co-Founder, Fury Biosciences LLC
Improving Expression and Stability of Immunocytokine Therapeutics
Davis Goodnight, PhD, Scientist II, A-Alpha Bio
The development of immunocytokine therapeutics is hindered by challenges with expression and stability. In this talk, we discussed using computational remodeling tools to create stable cytokine variants and high-throughput measurements to improve their functional expression. The resulting immunocytokines showed improved developability and elicited an anti-tumor response with limited toxicity in a mouse syngeneic tumor model.
Designing Tumor-Selective Multispecific Antibodies for the Treatment of Solid Tumors
The immunosuppressive tumor microenvironment in solid cancers has long been documented to be highly dysregulated, contributing broadly to tumor survival. Numerous cell surface markers and enzymatic activities have been correlated with poor disease outcomes. We take an unbiased approach to the discovery of novel cell surface markers and enzymatic activities that can be leveraged to design and build tumor selective multispecific immunotherapies.
Directed Assembly of Bispecific Antibody by Electrostatic Steering—Development of Platform and Application to Therapeutic Antibodies
Hitoshi Katada, PhD, Head, Biologics Engineering, Chugai Pharmaceutical Co. Ltd.
To address chain pairing when expressing bispecific antibodies, we have established FAST-Ig technology which promotes correct heavy- and light-chain assembly through electrostatic steering. In this presentation, development and application of FAST-Ig platforms including structural insight using two therapeutic antibodies will be introduced.
Alexi Cabatingan, Chromatography Resin Specialist Resin Specialist, Sales, Cytiva
Senthil Kumar, GoSilico Sales Specialist, Chromatography, Cytiva
Developing purification protocols for bispecific antibodies present extra challenges compared to conventional therapeutic monoclonal antibodies (mAbs). Strategies for efficient capture and polishing are discussed already in antibody engineering. The best combination of available resins and methods needs to provide sufficient separation of product and process related impurities. In this talk, we explore different purification strategies and see how in silico chromatography process development can streamline experimental PD work and simultaneously improve process understanding.
11:00 amNetworking Coffee Break
Engineering Solutions for Homogeneous Production of Asymmetric Bispecific Antibodies with the DuetMab Platform
John D. Bagert, PhD, Associate Director, Biologics Engineering, AstraZeneca
Asymmetric monovalent bispecific IgGs are becoming a leading biotherapeutic format, however, correct chain pairing remains a production challenge. Building on our clinically validated DuetMab platform, we present engineering solutions for streamlining the manufacturing of correctly assembled bispecific antibodies. We introduce novel electrostatic steering mutations and interchain disulfide engineering to facilitate orthogonal-chain pairing between heavy and light chains. We show the versatility of this platform for a diverse set of bsIgGs.
Trop2-Targeted CD28 Bi/Trispecific Antibodies Enhance T Cell Activation and Tumor-Cell Killing
Yoon Kyung Kim, PhD, Principal Scientist, Discovery Biology & Pharmacology, Xencor
T cell activation is initiated by TCR/CD3 binding to peptide-MHC and enhanced by co-stimulatory receptor engagement. Since solid tumors lack these ligands, we developed a bispecific antibody that bridges Trop2, an emerging target overexpressed on various solid tumors, to the CD28 co-stimulatory receptor on T cells. This presentation highlights preclinical data on Trop2-targeted CD28 co-stimulation combined with CD3 bispecific antibodies, aiming to prolong T cell survival and boost anti-tumor responses.
Jane Seagal, VP Antibody Discovery, Antibody Discovery, AlivaMab Biologics LLC
Efficient biologic therapeutic discovery and engineering relies on diverse, high-quality antibody libraries. Here we highlight the agility of AlivaMab Biologics and Ablexis platforms supported by a collection of AlivaMab® Mouse strains enabling the development of novel modalities, including fully human single-domain antibodies, a unique approach to CLC discovery, and TCRm antibodies. Our platforms consistently deliver molecules with the key attributes required for successful drug development.
12:45 pmSession Break
Chairperson's Remarks
Nick Till, PhD, Postdoctoral Fellow, Chemistry, Stanford University
Accelerating Lead ID: Navigating the bsAb ADC Discovery Landscape to Accelerate Drug Candidate Nomination
Nicholas Marshall, PhD, Head of Protein Sciences, Invenra Inc.
The potency and multi-target specificity advantages of bispecific antibody drug conjugates (bsAb ADC) differentiate them from traditional antibody therapeutics. The complexity of engineering bsAb ADC drugs is significant, and years may be spent optimizing for both efficacy and manufacturability. Using the B-Body bispecific platform, Invenra is able to validate target pairs and evaluate drug candidates simultaneously in a framework with proven manufacturability, thereby shortening the lead ID phase.
Tailoring Multispecifics for Context-Dependent Efficacy
Matthew Lundberg, PhD, Associate Director, Protein Engineering, Tentarix Biotherapeutics Inc.
Multispecific antibodies hold immense therapeutic potential. However, their efficacy can be hindered by non-specific activation. This talk will explore strategies to engineer multispecifics for context-dependent activation using Tentarix platform technologies, enhancing therapeutic index and minimizing off-target effects. By incorporating cell-specific targeting with receptor agonism, we aim to optimize multispecific antibodies for targeted and effective disease intervention.
Stefan Schmidt, PhD, CEO, evitria AG
Bispecific antibodies are currently the fastest growing segment of the antibody market. Selecting the antibody for binding is no longer sufficient as other parameters such as avidity, geometry, flexibility or spatial distance of the binders have a huge impact on the biological function. Therefore, a huge variety of formats has been developed. In this presentation we describe the manufacturing and comparison of a range of different versions and discuss properties and advantages of these antibodies.
3:35 pmNetworking Refreshment Break
App Workshop- Successful Tips for Navigating PepTalk App for your Onsite Experience
Kevin Brawley, Project Manager, Production Operations & Communications, Cambridge Innovation Institute
Julie Sullivan, Production, Cambridge Innovation Institute
Looking to maximize your onsite experience? Want to connect with fellow attendees? Need help viewing the app? Come join us for the App Workshop! We will have tips to navigating the app to maximize your onsite experience.
Joe JiuQiao Zhao, Head, External Innovation, Nona Biosciences
HCAb Harbour Mice® is a fully human immunoglobulin transgenic mouse platform that produces fully human heavy chain-only antibodies (HCAb). This presentation will explore the genesis and evolution of HCAb Harbour Mice®, highlighting the application of fully human VHH in bispecific and multi-specific antibodies, CAR-T therapies, ADCs, and mRNA-LNP therapeutics.
Trogocytosis-Targeting Chimeras (TrogoTACs) for Targeted Protein Transfer
Multiple methods for degrading cell surface proteins have been reported over the past several years, but directly introducing cell surface proteins without genetic intervention remains challenging. Herein we disclose the development of bispecific molecules (TrogoTACs) capable of inducing contact-dependent membrane transfer between cells by redirecting trogocytosis in a targeted fashion. To accomplish this goal, chimeric antibody–small molecule conjugates were designed with specificity to cell surface proteins displaying mutually exclusive expression on donor and acceptor cell types. The protein transfer process is rapid, requires cell-cell contact, and depends on expression of the receptors targeted by the TrogoTAC.
Generation of Multispecific WNT Mimetics for Tissue Regeneration
Hui Chen, PhD, Associate Director, Protein Sciences, Surrozen
WNTs regulate myriad biological processes during embryonic development and are key regulators of stem cell function, tissue homeostasis, and injury repair in adults. However, it is very challenging to develop WNT molecules into therapeutic molecules due to their hydrophobic properties. We described a platform for potent, selective WNT surrogate generation by multivalent binding to Frizzleds (FZDs) and low-density lipoprotein receptor–related proteins (LRPs). Recently, we further explored a cell-targeting system we have termed BRAID (BRidged Activation by Intra/intermolecular Division) for cell-specific targeting.
Dual Antibody Inhibition of KLK5 and KLK7 for Netherton Syndrome and Atopic Dermatitis
Cecilia Chiu, PhD, Staff Scientist I, Genentech, Inc.
Serine proteases kallikreins KLK5 and KLK7 are critical for maintaining skin barrier function. Excessive KLK activities can lead to Netherton syndrome and atopic dermatitis. Our study demonstrated that combined treatment with inhibitory anti-mKLK5 and anti-mKLK7 antibodies improves skin integrity and reduces inflammation in mouse NS and AD models. We further generated a humanized bispecific aKLK5/7 inhibitory antibody, presenting a promising therapy for clinical development in NS and other inflammatory dermatoses.
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