# Overcoming limitations for AAV gene therapy

> **NIH NIH P50** · UNIVERSITY OF WASHINGTON · 2024 · $669,685

## Abstract

Gene therapy is a promising treatment for the muscular dystrophies. Our Center has played major roles in
advancing the use of AAV for muscle disease. These include extensive characterization of dystrophin and DUX4
expression and function, the discovery that AAV can be used for systemic gene delivery to muscle, and
generation of numerous small, muscle-specific expression cassettes (MSECs), micro-dystrophins (μDys) and
RNAi cassettes. These advances have enabled multiple gene therapy trials for DMD, LGMDs, XL-MTM1and
other muscle disorders. We have also developed and advanced many skeletal and cardiac muscle testing
platforms and tools useful for muscle gene therapies, including 3D DMD human iPSC-derived engineered muscle
tissues and a DMD rat model. However, current AAV- μDys therapies are not as effective as hoped, and AAV-
RNAi therapies for FSHD and other dominant disorders have not advanced to the clinic. Here we propose two
related aims to address limitations of AAV gene therapies: (A) Testing new AAV capsid variants for cardiac and
skeletal muscles, iterative testing of novel micro-dystrophins, larger split-intein dystrophins, and MSEC designs
to minimize immunogenicity and increase cardiac and skeletal muscle potency; (B) Application of enhanced
cassettes and vectors for DUX4 transcript knock-down in FSHD therapy. In Aim 1, we develop vectors to improve
DMD clinical interventions that have been limited by the levels and functionality of therapeutic dystrophins, and
by very high vector doses that have caused serious adverse events (SAEs) in some patients due to
immunological reaction to the vector and/or transgene. We will compare multiple myotropic serotypes, which
show significantly increased muscle transduction to deliver novel transgene cassettes that have been designed
for reduced immunogenicity and increased potency, especially in cardiac muscle. A major focus will include the
testing of novel, split-intein AAV vectors to produce mini- and full-length dystrophins. We also test a dual vector
strategy to recover depressed function in the heart via overexpression of an enzyme (RNR) that elevates cardiac
dATP, a small molecule myosin activator. Studies of immune response to dystrophin will be augmented by
screening patient blood cells for immune reactivity. In Aim 2 we combine the myotropic vectors with enhanced
RNAi cassettes to advance gene therapy for FSHD. This experimental plan combines vector developments from
Aim 1 with new FSHD animal models and FSHD clinical studies from Project 2. Genetic and phenotypic changes
in the FLExDUX4 mouse model of FSHD will be targeted via local and systemic delivery of AAV-DUX4 RNAi,
while further studies will evaluate these AAV-DUX4 RNAi vectors in the Göttingen minipig model of FSHD that
is being characterized in Project 2. DUX4 gene silencing and reduction of inflammation in the minipig will be
measured by MRI, muscle structural changes, and biomarkers based on clinical results from Project 2. Toge...

## Key facts

- **NIH application ID:** 10922780
- **Project number:** 5P50AR065139-11
- **Recipient organization:** UNIVERSITY OF WASHINGTON
- **Principal Investigator:** JEFFREY S CHAMBERLAIN
- **Activity code:** P50 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $669,685
- **Award type:** 5
- **Project period:** 2014-05-07 → 2028-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10922780

## Citation

> US National Institutes of Health, RePORTER application 10922780, Overcoming limitations for AAV gene therapy (5P50AR065139-11). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/10922780. Licensed CC0.

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