2025 ARCHIVES

Cambridge Healthtech Institute’s Inaugural

Emerging Oligonucleotide Modalities

Pursuing Circular RNA, tRNA, and Innovative Editing Approaches

March 11 - 12, 2025 ALL TIMES EDT

Cambridge Healthtech Institute’s inaugural conference on Emerging Oligonucleotide Modalities shines light on the incredible creativeness of chemists and biologists in designing new targeted therapies. Equipped with innovative engineering tools and delivery mechanisms, scientists are modifying naturally occurring tRNAs, circular RNAs, and non-coding RNAs, and using editing tools to overcome some of the limitations in existing oligo therapies. The talks highlight some of the newer oligo modalities that are showing a lot of promise in terms of improving efficacy, stability, toxicity, and frequency of administration.

Tuesday, March 11

8:00 amRecommended Short Course*

SC1: Safety & Toxicity of Nucleic Acids
*Premium Registration or separate registration required. See Short Courses page for details.

9:45 amRegistration and Morning Coffee

10:45 amWelcome Remarks by Conference Organizer

10:55 am

Chairperson's Remarks

Paloma Giangrande, PhD, Senior Vice President, Discovery and Translational Biology, Orbital Therapeutics

11:00 am

Circular RNA: Transforming a Promising Technology into Cutting-Edge Therapeutics

Edo Kon, PhD, Director of Business Development, RiboX Therapeutics

RiboX Therapeutics is a globally-operated biotech company focusing on discovering and developing fully engineered circular RNA as a therapeutic modality, which offers advantages to address key challenges of mRNA medicines. RiboX has established a plug-and-play circular RNA platform, an ionizable lipid platform, and has unique assets in active targeting LNP under development.

11:30 am

Circular mRNA and Its Application in Immunotherapy and Genome Engineering

Li Li, PhD, Assistant Professor, RNA Therapeutics Institute, University of Massachusetts Chan Medical School

Circular mRNA (CircRNA) has generated substantial interest as a new mRNA therapeutics platform. Here I will discuss a scalable and column-free method for preparing non-immunogenic circular mRNAs. I will also show its applications in immunotherapy and genome editing.

12:00 pm

The Therapeutic Potential of circRNAs: Their Stability, Abundance, and Unique Properties

Gilles Besin, PhD, CSO, Orbital Therapeutics

Circular RNAs (circRNAs) are a class of non-coding RNAs that form a covalently closed loop structure, meaning they do not have 5' to 3' polarity or a poly-A tail, unlike linear RNAs. Initially thought to be byproducts of splicing errors, circRNAs are now recognized as important regulatory molecules in various biological processes. They can act as microRNA sponges, regulate transcription, interact with proteins, and potentially even encode peptides in some cases.The therapeutic potential of circRNAs has gained increasing attention due to their stability, abundance, and unique properties.

12:30 pmEnjoy Lunch on Your Own

1:50 pm

Chairperson's Remarks

Paloma Giangrande, PhD, Senior Vice President, Discovery and Translational Biology, Orbital Therapeutics

1:55 pm

FEATURED PRESENTATION: Design and Delivery of tRNA Therapeutics to Treat Stop Codon Disease

William Kiesman, PhD, CTO, Alltrna

This talk will explore designing, manufacturing, and delivering transfer RNA (tRNA) as a new therapeutic modality. We will examine how this innovative technology can be applied across diseases caused by a premature termination codon (PTC), collectively referred to as Stop Codon Disease, and discuss initial proof-of-concept experiments to unlock the potential in tRNA biology to create a universal precision medicine to treat diseases with shared genetic mutations.

2:25 pm PANEL DISCUSSION:

Emerging Modalities and Technologies for Developing Oligo Therapeutics

PANEL MODERATOR:

Paloma Giangrande, PhD, Senior Vice President, Discovery and Translational Biology, Orbital Therapeutics

PANELISTS:

Gilles Besin, PhD, CSO, Orbital Therapeutics

Neil Kubica, PhD, Therapeutics Division Lead, General Inception

David Mauger, PhD, Head, Data Science, Ascidian Therapeutics

Sriram Sathy, PhD, CSO, AIRNA Corp.

Basheer Zada, Principal, EcoR1 Capital, LLC

3:25 pmGrand Opening Refreshment Break in the Exhibit Hall with Poster Viewing

4:10 pm

Organizer's Welcome Remarks

Gemma Smith, Senior Conference Director, Production, Cambridge Healthtech Institute

4:15 pm

Plenary Chairperson's Remarks

Dmitry Samarsky, PhD, CSO and Board Member, GALconda Therapeutics

4:20 pm

siRNA Chemical Engineering

Anastasia Khvorova, PhD, Professor, RNA Therapeutic Institute, University of Massachusetts Medical School

The focus of our lab is to identify, characterize, and develop novel chemistries that promote simple, efficient, and non-toxic delivery of oligonucleotides and potent silencing of therapeutic targets in vivo. Some examples will be highlighted in this talk.

5:00 pm

TANGO: An RNA Splicing Approach to Upregulate Proteins

Edward Kaye, MD, CEO and Director, Stoke Therapeutics

Targeted Augmentation of Nuclear Gene Output (TANGO) is an RNA splicing approach that enables the upregulation of many proteins. Specifically designed Anti-sense Oligonucleotides (ASOs) splice out retained naturally occurring 'poison exons' or NMD exons from pre-mRNA, thus enabling an increase of full-length message and full-length protein. We are targeting autosomal dominant diseases which are missing 50% of an essential protein to correct the underlying genetic defect.

5:40 pm10th Annual Welcome Reception in the Exhibit Hall with Poster Viewing

6:50 pmClose of Day

Wednesday, March 12

7:30 amRegistration and Morning Coffee

8:00 am

Chairperson's Remarks

Jaspreet Khurana, PhD, Senior Director, mRNA Programming, Strand Therapeutics, Inc.

8:05 am

RNA Activation in Cancer and Rare Genetic Diseases

Nagy Habib, ChM, FRCS, Professor of Surgery, Imperial College London

RNA activation with small activating RNAs can lead to upregulation of transcription in the nucleus resulting in increased mRNA and targeted protein. Such activation is specific and can last about a month This can be applied to many genes down regulated in common conditions such as cancer as well as rare genetic diseases such as sickle cell disease. Bio-distribution can be performed either with a universal or more targeted delivery approach. Wide bio-distribution is suitable in rare genetic diseases as well as with diseases related to the dark genome where the reduced long noncoding RNA is tissue, cell, and status specific.

8:35 am

Engineered Inhibitory tRNAs as Novel Therapeutics for Oncology

Austin Draycott, PhD, CEO, Cloverleaf Bio

At Cloverleaf Bio, we are developing a new class of engineered tRNA therapeutics. Our tRNAs target an underappreciated vulnerability of cancer: addiction to high levels of tRNA modifying enzymes. Cloverleaf’s approach to drugging tRNA modifying enzymes uses engineered “trojan horse” tRNAs. The programmability, potency, and specificity of our tRNAs will potentially improve cancer treatment across a range of indications.

9:05 am

KEYNOTE PRESENTATION: miRNA-Based Logic Circuits Encoded on Self-Amplifying RNA for Highly Specific Cancer Cell Classification

Ron Weiss, PhD, Professor, Biological Engineering, Massachusetts Institute of Technology

We developed self-amplifying RNA and modified RNA platforms into vectors capable of carrying synthetic circuitry payloads that can provide a variety of desirable dynamics. We also encoded miRNA target sites on our RNA vectors to provide for highly specific cell type classification. We are using this technology to create next-generation cancer immunotherapy RNA vectors capable of activating therapeutic payloads discriminately in cancer cells.

9:35 amCoffee Break in the Exhibit Hall with Poster Viewing

10:15 am

Advancing Cancer Immunotherapy with mRNA Synthetic Biology

Jaspreet Khurana, PhD, Senior Director, mRNA Programming, Strand Therapeutics, Inc.

We have developed a platform in which we design RNA-encoded programmable genetic “circuits” that detect molecular cues in a cell to specifically express a payload protein in cells that exhibit a particular molecular signature. We applied this platform to the development of our program which entails systemic delivery of lipid nanoparticle (LNP)–encapsulated mRNA-bearing programmable genetic circuitry that selectively expresses a therapeutic payload within target cells.

10:45 am

Mimicking Retroviral Replicative Complexes Using Optimized TLR7/8/9 Agonists for Cancer Immunotherapy

Arthur Krieg, MD, Founder, President and Acting CEO/CSO, Zola Therapeutics

A CpG-A DNA TLR9 agonist in a virus-like particle, vidutolimod, induces systemic tumor regression as a monotherapy in PD-1 refractory advance melanoma, which is associated with the secretion of IFN-a. We have now developed native backbone GU-rich RNA TLR7/8 agonists formulated in lipid nanoparticles that are stronger inducers of IFN-a secretion compared to CpG-A DNA, and which show synergy when used in combination. IV delivery of TLR7/8/9 agonists is well tolerated in mice and nonhuman primates, and induces pharmacodynamic biomarkers associated with human clinical response. Plans for clinical development will be discussed.

11:30 amLunch in the Exhibit Hall

12:40 pm

Plenary Chairperson's Remarks

Michael Byrne, PhD, VP Research Pharmacology, Research Pharmacology, WAVE Life Sciences

12:45 pm

Delivery with Bicycles and Camelids: Targeted Delivery of Oligonucleotide Drugs to Muscle and the Central Nervous System via the Transferrin Receptor

Eric Swayze, PhD, Executive Vice President, Research, Ionis Pharmaceuticals

Ligands for transferrin receptor can potentially provide solutions to the delivery of oligonucleotides to skeletal and cardiac muscle, as well as across the blood brain barrier. We have optimized oligonucleotide conjugates to TfR1 ligands including Bicycle peptides and camelid nanobodies to reduce the total dose of the administered drug. These constructs have achieved successful delivery to the target tissues, offering the potential for treatment of cardiovascular and neurological diseases.

1:25 pm

CRISPR Genome Editing for Therapeutic Applications: Advances in in vivo Editing

Ramsey Majzoub, PhD, Director, Intellia Therapeutics

At Intellia, we are advancing a full-spectrum genome editing company. We are deploying the industry’s broadest and deepest toolbox, including novel editing and delivery solutions, to harness the immense power of CRISPR-based technologies for in vivo and ex vivo therapeutic applications. In this presentation, we will share the advances in the therapeutic applications of CRISPR/Cas9 for in vivo genome editing.

2:05 pmRefreshment Break in the Exhibit Hall with Last chance for Poster Viewing

2:40 pmIn-Person Breakout Discussions

Breakout 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/s 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 Breakout Discussion page on the conference website for a complete listing of topics and descriptions.

IN-PERSON ONLY BREAKOUT DISCUSSION: Designing and Optimizing New RNA Modalities as Therapeutics

Gilles Besin, PhD, CSO, Orbital Therapeutics

William Kiesman, PhD, CTO, Alltrna

Edo Kon, PhD, Director of Business Development, RiboX Therapeutics

Li Li, PhD, Assistant Professor, RNA Therapeutics Institute, University of Massachusetts Chan Medical School

Innovative circular RNAs and their applications
Optimizing tRNA design and delivery
Developing Self-amplifying and programmable RNAs
Establishing criteria for modality selection, application and success

3:25 pm

Chairperson's Remarks

Jonathan Watts, PhD, Professor, RNA Therapeutics Institute, University of Massachusetts Chan Medical School

3:30 pm

Therapeutic Applications for Hepatic and Extrahepatic RNA Editing via Endogenous ADAR Enzymes

Ian Harding, PhD, Senior Scientist I, Wave Life Sciences

AIMers are oligonucleotides that engage endogenous ADAR enzymes to induce highly efficient and specific A-to-I RNA base editing. Our recently optimized AIMer design increases the potency, target space, and tissue targeting capabilities of RNA editing. Optimized AIMers support efficient RNA editing in both hepatic and extrahepatic tissues, including the central nervous system, kidney, and lung. We will show that AIMers support RNA editing of disease-relevant targets in multiple tissues.

4:00 pm

Characterization of Oligo Directed RNA Editing with Purified ADAR Proteins

Shanhu Hu, PhD, Director, Platform Biology, Korro Bio Inc.

This talk will discuss the successful purification of human full-length and active ADAR1 and ADAR2 proteins and how it enables mechanistic understanding of oligo mediated RNA editing.

4:30 pm

Approaches to Optimize Safety and Potency of LNP-Based CRISPR-Based Medicines Delivered In Vivo

Steven Wolk, PhD, President, Sinawali Biotechnology Solutions

The goal for the next generation of CRISPR-based medicines is the development of potent and safe therapeutics that can be delivered in vivo specifically to the target cells of interest. The mRNA/LNP format is currently showing the most promise to achieve this challenging goal, and various factors can be optimized to enhance performance, including vehicle (lipid composition and targeting elements), cargo (mRNA and gRNA), and analytical method development.

5:00 pmClose of Conference