Page 65 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

Appendix B

Workshop Agenda

Advancing Gene-Targeted Therapies for
Central Nervous System Disorders: A Workshop

April 23–24, 2019
National Academy of Sciences Building
2101 Constitution Avenue, NW
Washington, DC

Background:

This public workshop will bring together experts and key stakeholders from academia, government, industry, and nonprofit organizations to explore approaches for advancing the development of gene-targeted therapies for central nervous system (CNS) disorders, including approaches that target nucleic acids, such as adeno-associated viruses (AAVs), antisense oligonucleotides (ASOs), and RNA interference, as well as gene product-targeted therapies.

Workshop Objectives:

Invited presentations and discussions will be designed to:

Provide an overview of the current landscape of gene-targeted therapy approaches for CNS disorders.

Page 66 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

Discuss lessons learned from recent advances in gene therapy and ASO development for retinal dystrophy and spinal muscular atrophy (SMA).
Compare features of different gene-targeted therapy approaches in development for CNS disorders, and discuss approaches to matching the approach to specific diseases; addressing their respective administration, distribution, and dose challenges; and exploring potential long-term effects.
Explore clinical development—including biomarker and clinical endpoint selection, trial design to demonstrate disease modification, and the regulatory path—for gene-targeted therapy approaches for rare genetic disorders that have more variable onset and slower progression.
Discuss what it would take to move beyond rare genetic disorders to develop gene-targeted therapy approaches for more common, heterogeneous disorders such as Alzheimer’s and Parkinson’s diseases.
Explore opportunities for catalyzing development of gene-targeted therapy approaches for nervous system disorders, including potential collaborative efforts among sectors and across disorders.

April 23, 2019

1:30 p.m.	Welcome and Overview of Workshop
	STORY LANDIS, Co-Chair, Forum on Neuroscience and Nervous System Disorders (Co-Chair)
	LAMYA SHIHABUDDIN, Sanofi (Co-Chair)

SESSION I: CURRENT LANDSCAPE AND LESSONS LEARNED

Objectives:

Provide an overview of the current landscape of gene-targeted therapy approaches for central nervous system disorders.
Explore lessons learned from gene and ASO therapies that have achieved Food and Drug Administration approval—including translation plans and which animal models were used in preclinical studies, use of dog models for RPE65, role of natural history studies for SMA therapy, and other lessons learned in translation to clinical development.

Page 67 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

Examine lessons learned from gene therapy efforts that were not successful, including neurotrophins for neurodegenerative diseases.

1:40 p.m.	Session Overview
1:40 p.m.	LAMYA SHIHABUDDIN, Sanofi (Moderator)
1:45 p.m.	RPE65 Gene Therapy
1:45 p.m.	KATHLEEN REAPE, Spark Therapeutics
2:00 p.m.	ASO Therapy for SMA
2:00 p.m.	C. FRANK BENNETT, Ionis
2:15 p.m.	Gene Therapy for SMA
2:15 p.m.	PETRA KAUFMANN, AveXis
2:30 p.m.	Lessons Learned from Unsuccessful Gene Therapy Trials of Neurotrophins for Neurodegenerative Diseases
2:30 p.m.	JEFFREY KORDOWER, Rush University
2:45 p.m.	Panel Discussion: Preclinical Studies, Delivery Methods, and Clinical Trial Issues Focused on These Cases with the Intent to Identify General Issues That Will and Will Not Apply to Other Applications/Diseases
	The speakers above will be joined by panelists:
	RONALD CRYSTAL, Weill Cornell Medicine
	CHRISTOPHER HENDERSON, Biogen
3:25 p.m.	General Discussion
3:45 p.m.	BREAK

SESSION II: SELECTING GENE-TARGETED THERAPY APPROACHES FOR CNS DISORDERS

Objectives:

Discuss the promise and potential pitfalls of gene-targeted therapies specifically for CNS disorders.
For CNS disorders, compare features of different therapies that target nucleic acid, including AAVs, ASOs, and RNA interference, as well as gene product–targeted therapies.

Page 68 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

Explore what makes a CNS disorder potentially amenable to treatment via gene-targeted therapies and how to match therapy modality and mechanism of action to specific diseases.
Discuss when uncontrolled overexpression is appropriate.

4:00 p.m.	Session Overview
4:00 p.m.	BEVERLY DAVIDSON, Children’s Hospital of Philadelphia and University of Pennsylvania School of Medicine (Moderator)
4:05 p.m.	Speakers
	ANASTASIA KHVOROVA, University of Massachusetts Medical School
	ASA ABELIOVICH, Prevail Therapeutics
	SARAH DEVOS, Denali Therapeutics
4:35 p.m.	Panel Discussion Among Speakers Above
5:00 p.m.	General Discussion
*Day One Closing Talk*
5:30 p.m.	The Vista for Developing Gene-Targeting Therapies for Psychiatric and Other Circuit Disorders
5:30 p.m.	STEVEN HYMAN, The Broad Institute
5:45 p.m.	Discussion
6:00 p.m.	ADJOURN DAY ONE

April 24, 2019

8:30 a.m.	Welcome and Overview of Day One
	STORY LANDIS, Co-Chair, Forum on Neuroscience and Nervous System Disorders (Co-Chair)
	LAMYA SHIHABUDDIN, Sanofi (Co-Chair)

Page 69 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

SESSION III: GENE-TARGETING THERAPY TECHNOLOGIES FOR CNS DISORDERS

Objectives:

For different therapy modalities, and with a focus on general issues rather than specific disease indications:
- Discuss approaches to addressing their respective administration challenges;
- Explore CNS fluid dynamics and barriers, as well as delivery routes and distribution, and dose; and
- Examine what is known about clinical and non-clinical safety, as well as potential long-term effects.
Consider how previously successful approaches for spinal muscular atrophy and retinal dystrophy would need to be adapted for monogenetic disorders that have more variable onset and slower progression, and discuss timing of interventions.
Discuss what it takes to move beyond monogenetic disorders to develop gene therapy approaches for common, heterogeneous disorders such as Alzheimer’s and Parkinson’s diseases.
Examine key challenges such as:
- CNS cell type-specific transduction;
- Regulation of viral gene expression to optimize safety and efficacy; and
- Capsid engineering to improve tissue-specific targeting and blood–brain barrier penetration.

8:40 a.m.	Session Overview
	DAVID BREDT, Janssen R&D (Co-Moderator)
	HAO WANG, Takeda Pharmaceuticals (Co-Moderator)
8:45 a.m.	Speakers
	BEVERLY DAVIDSON, Children’s Hospital of Philadelphia and University of Pennsylvania School of Medicine
	JUNGHAE SUH, Rice University
	VIVIANA GRADINARU, California Institute of Technology
	JUDE SAMULSKI, University of North Carolina School of Medicine
9:25 a.m.	Panel Discussion
9:45 a.m.	General Discussion

Page 70 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

10:15 a.m.

BREAK

SESSION IV: CLINICAL TRIAL DESIGN AND REGULATORY PATHWAYS

Objectives:

Translation and treatment paradigm: Explore issues with preclinical models, delivery, considerations for first-in-human, immune response, dose–response, and dose and dose regimen selection. What unique challenges do neuropsychiatric diseases present?
Patient access: Discuss recruitment challenges, natural history studies, and opportunities with registries/patient advocacy.
Regulatory pathway: Address ethical considerations, issues with standards and harmonization, and overall level of proof required.
Risk/benefit and value to patients: Consider how to define meaningful, clinically relevant endpoints, and how to demonstrate efficacy, safety, and overall effectiveness over the long run.
- Specific questions may include: Should long-term toxicity studies be required (6 months or more)? Should biodistribution and rationale be considered for each gene product or can biosimilars be cross-referenced? What is a biosimilar?

10:30 a.m.	Session Overview
10:30 a.m.	DANIEL BURCH, PPD Biotech (Moderator)
10:35 a.m.	Translation
10:35 a.m.	AKSHAY VAISHNAW, Alnylam
10:45 a.m.	Clinical
	MICHAEL PANZARA, Wave Biosciences
	CRISTINA SAMPAIO, CHDI Foundation
11:05 a.m.	Regulatory Pathway
	PETER MARKS, Food and Drug Administration
	RUNE KJEKEN, Norwegian Medicines Agency
11:25 a.m.	Ethics
11:25 a.m.	HOLLY TABOR, Stanford University
11:35 a.m.	Patient Advocacy
11:35 a.m.	TIM COETZEE, National Multiple Sclerosis Society

Page 71 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

11:45 a.m.	General Discussion
12:30 p.m.	LUNCH

SESSION V: MOVING FORWARD

Objectives:

Discuss new technologies on the horizon, for example, non-viral approaches, small molecules targeting RNA (e.g., ExpansionRx, Arrakis, Skyhawk), chaperones, targeted protein degradation (many companies), and cell penetrant stapled peptide therapeutics (e.g., Fog Pharma).
How can these approaches be used for psychiatric disorders and other circuit disorders?
What else do we need to know that we do not know? Examples may include precision medicine for low-incidence disorders, developing a strategic pipeline for treatments, Timothy syndrome, and/or neuregulins.
Briefly discuss issues related to cost, access, and health equity, as well as AAV manufacturing capacity.

1:30 p.m.	Session Overview
	FRANCES JENSEN, Perelman School of Medicine, University of Pennsylvania (Moderator)
1:35 p.m.	Gene Mutations in Autism and Associate Neurodevelopmental Disorders
	JOSEPH BUXBAUM, Icahn School of Medicine at Mount Sinai
1:50 p.m.	Novel, Non-Viral Methods of Gene Therapy, Tunable Vectors, and AAV Manufacturing Capacity
	ROBERT KOTIN, Generation Bio and University of Massachusetts Medical School
2:05 p.m.	Using a Small-Molecule Drug to Modulate Splicing
	ANU BHATTACHARYYA, PTC Therapeutics
2:20 p.m.	Non-Viral Delivery Nanoplatforms for Brain-Targeted Genome Editing
	SHAOQIN SARAH GONG, University of Wisconsin–Madison

Page 72 Cite

Suggested Citation:"Appendix B: Workshop Agenda." National Academies of Sciences, Engineering, and Medicine. 2019. Advancing Gene-Targeted Therapies for Central Nervous System Disorders: Proceedings of a Workshop. Washington, DC: The National Academies Press. doi: 10.17226/25529.

×

2:35 p.m.	Cost, Access, and Equity Issues
2:35 p.m.	HOLLY TABOR, Stanford University
2:50 p.m.	Panel Discussion
3:05 p.m.	General Discussion
3:45 p.m.	Synthesis of Key Workshop Themes and Future Directions
	STORY LANDIS, Co-Chair, Forum on Neuroscience and Nervous System Disorders (Co-Chair)
	LAMYA SHIHABUDDIN, Sanofi (Co-Chair)
4:00 p.m.	ADJOURN WORKSHOP