Pompe disease is a fatal neuromuscular disorder that results from mutations in the gene encoding acid ?-glucosidase (GAA) - an enzyme necessary for lysosomal glycogen hydrolysis. Hypoventilation and respiratory insufficiency are prominent features of Pompe disease that result in respiratory failure in untreated infants. Although breathing problems have traditionally been attributed to respiratory muscle and motor neuron pathology, we recently described the significant role of smooth muscle (SM) pathology in the respiratory- related morbidity of this disease. Currently, the only FDA approved therapy available to Pompe patients is enzyme replacement therapy (ERT). ERT has significantly increased survival but as patients live longer, life threatening SM pathology such as ruptured vascular aneurysms and airway weakness, has been unmasked. The extent of residual SM involvement and cellular dysfunction following ERT remains unknown and will be a focus of this project. In addition, we will study the efficacy of adeno-associated viral (AAV) gene therapy in treating Pompe SM involvement. AAV gene therapy is ideal for monogenetic disorders such as Pompe disease, however evidence of an AAV for infantile Pompe disease that targets SM, skeletal, cardiac and motor neurons is still lacking. We propose a series of pre-clinical experiments that directly address SM lysosomal glycogen accumulation in Pompe disease and explore the efficacy of AAV vectors in targeting all affected muscle groups and motor neurons. We will focus on an AAV serotype and promoter that targets SM lysosomal glycogen accumulation as well as cardiac, skeletal and motor neuron pathology in Pompe disease. Overall, the fundamental hypothesis driving this proposal is that extensive smooth muscle glycogen accumulation persists in Pompe disease despite ERT and that a novel AAV vector is necessary to treat smooth, skeletal, cardiac, and motor neuron pathology. Our hypothesis has been formulated based on preliminary data in the Pompe disease mouse model as well as clinical evidence seen in our Pompe disease patients.
Three specific aims will be accomplished using an established mouse model of Pompe disease:
Aim 1 : To comprehensively examine respiratory and vascular SM involvement in Pompe disease and the impact of this pathology on autophagic dysregulation.
Aim 2 : To compare early and late ERT on respiratory and vascular SM function and glycogen accumulation.
Aim 3 : To examine the ability of a novel rationally designed AAV8g9-GAA to effectively transduce and clear SM, skeletal muscle, and motor neuron glycogen accumulation in comparison to AAV8 and AAV9. This project will address a gap in knowledge regarding smooth muscle dysfunction and will identify the potential of a novel AAV therapy for infantile Pompe disease to significantly reduce morbidity and mortality.

Public Health Relevance

Infantile Pompe disease is a fatal neuromuscular disorder associated with deficiency of an enzyme (acid alpha glucosidase) which is required to degrade glycogen. This deficiency occurs in the heart, smooth and skeletal muscle and neurons. It results in many problems including breathing difficulties, brain aneurysms and strokes. The only FDA approved treatment is enzyme replacement therapy (ERT). ERT has significantly increased survival but as patients live longer life threatening smooth muscle pathology has been unmasked. This application aims to comprehensively examine smooth muscle involvement with and without ERT and target the global disease ? cardiac, skeletal and smooth muscle as well as respiratory neurons - using adeno-associated virus gene therapy.

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
1R01HD099486-01
Application #
9800805
Study Section
Gene and Drug Delivery Systems Study Section (GDD)
Program Officer
Parisi, Melissa
Project Start
2019-09-12
Project End
2024-05-31
Budget Start
2019-09-12
Budget End
2020-05-31
Support Year
1
Fiscal Year
2019
Total Cost
Indirect Cost
Name
Duke University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705