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
Jay Sarkar, PhD, CoFounder, reThink64 Bionetworks
Discovery of a New Class of Cell-Penetrating Peptides by Novel Phage Display Platform
Jinsha Liu, PhD, Senior Scientist, Tentarix Biotherapeutics
A novel phage display platform, NNJA, was developed for targeted and cytosolic delivery. This innovative approach involves engineering a lysosomal cathepsin substrate into phage PIII, which displays a unique random sequence at its N-terminus. By selectively eliminating lysosomal-trapped peptide-phage, NNJA enables peptide-phage that escapes lysosomes to advance to the next round. Proof-of-concept studies demonstrated efficient cytosolic siRNA delivery by NNJA peptides, leading to significant gene silencing across various cell types. The NNJA platform offers a highly efficient discovery engine for targeted delivery to cytosol.
Conjugation of Antibodies to Lipid Nanoparticles for Enhanced Target Localization
QC Yong, PhD, Associate Director, Antibody CMC, Capstan Therapeutics
Antibody-conjugated lipid nanoparticles (LNPs) are developed to enhance targeted drug delivery. By coupling antibodies to LNPs, we aim to improve therapeutic efficacy and reduce off-target side effects through precise localization to target cells.
Bioreversible Anionic Bioconjugation for Intracellular Protein Delivery
Azmain Alamgir, Research Scientist, Biochemical Engineering, Cornell University
Intracellular protein delivery is challenging due to cellular barriers. We developed a novel bioconjugation method to introduce anionic groups onto proteins, enhancing their encapsulation in lipid nanoparticles. This approach enables efficient intracellular protein delivery with potential for broad therapeutic applications.
10:30 amNetworking Coffee Break
Quantitation and Integrity Evaluation of RNA Genome in Lentiviral Vector by Direct RT-ddPCR
Zhiyong He, PhD, Biologist, R&D, NIST
Lentiviral vectors (LV) are powerful tools for cell and gene therapies. We have developed a direct reverse transcription digital droplet PCR (RT-ddPCR) approach without RNA extraction and purification for estimation of LV titer and genome integrity. The advantage of direct RT-ddPCR is to avoid the RNA extraction and handling. Our results showed that direct RT-ddPCR resulted in the equivalent titers determined by RNA extraction followed by RT-ddPCR.
Molecular Exclusion Limits for Diffusion Across a Porous Capsid
Ekaterina Selivanovitch, PhD, Postdoctoral Researcher, Cornell Smith School of Chemical and Biomolecular Engineering, Cornell University
We investigated the size limitations for molecules diffusing through a porous protein capsid. By encapsulating enzymes and varying the size of substrates, we determined the effective pore size and identified factors influencing molecular transport across the capsid.
12:15 pmEnjoy Lunch on Your Own
12:45 pmSession Break
Chairperson's Remarks
Optimization of Biocompatibility for a Hydrophilic Biological Molecule Encapsulation System
Nathaniel Nucci, PhD, Associate Professor, Biological and Biomedical Sciences, Rowan University
Reverse micelle (RM) encapsulation has long been an attractive mechanism for biological delivery, yet an RM-based platform has yet to show generalized success for biocompatible encapsulation and delivery of drugs. We use RMs to encapsulate proteins for structure/function study. Recently, we have worked to leverage what works well for structural studies toward development of a biocompatible platform for protein encapsulation and delivery. Our most recent developments will be presented.
Versatile Cell/Tissue-Specific Delivery of AAV9 with No Capsids Engineered at All
Junichi Takagi, PhD, Professor, Institute for Protein Research, Osaka University
Development of AAV vectors with defined tissue tropism usually employs capsid engineering, often by inserting targeting peptides into capsid loops. However, engineered capsids with unique tissue tropism often show poor physicochemical properties that raise concerns in transduction efficiency, manufacturability, and safety. I will introduce a new method we have developed recently that can grant receptor-specific tissue tropism to natural and unmodified AAV9 capsids. This technology was used to achieve enhanced brain delivery of AAV9 in mice.
3:05 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.
Harnessing Exosomes for Delivery of Therapeutic Proteins and Nucleic Acids
Pranav Sharma, PhD, Founder & CSO, R&D, Xosomix
Novel Nanoscale Drug Eluting Stents for Large-Molecule Delivery
The limited uptake of nanoparticle carriers has restricted the applications of new drug modalities like RNAs, DNA, and peptides. Instead of relying on endocytotic uptake, our novel nanoscale drug eluting stent constructs connect into the nanotube networks between cells, then channel large drug cargoes into their cytoplasm. Here, we present their unique properties and their utility in delivering a variety of drug modalities and to a variety of cells/tissues.
Breaking Barriers: Next-Generation Vectors for Protein Therapeutics
Programs