Litcius/Paper detail

Gene Therapy Developments for Pompe Disease

Zeenath Unnisa, John K. Yoon, Jeffrey W. Schindler, Chris Mason, Niek P. van Til

2022Biomedicines50 citationsDOIOpen Access PDF

Abstract

Pompe disease is an inherited neuromuscular disorder caused by deficiency of the lysosomal enzyme acid alpha-glucosidase (GAA). The most severe form is infantile-onset Pompe disease, presenting shortly after birth with symptoms of cardiomyopathy, respiratory failure and skeletal muscle weakness. Late-onset Pompe disease is characterized by a slower disease progression, primarily affecting skeletal muscles. Despite recent advancements in enzyme replacement therapy management several limitations remain using this therapeutic approach, including risks of immunogenicity complications, inability to penetrate CNS tissue, and the need for life-long therapy. The next wave of promising single therapy interventions involves gene therapies, which are entering into a clinical translational stage. Both adeno-associated virus (AAV) vectors and lentiviral vector (LV)-mediated hematopoietic stem and progenitor (HSPC) gene therapy have the potential to provide effective therapy for this multisystemic disorder. Optimization of viral vector designs, providing tissue-specific expression and GAA protein modifications to enhance secretion and uptake has resulted in improved preclinical efficacy and safety data. In this review, we highlight gene therapy developments, in particular, AAV and LV HSPC-mediated gene therapy technologies, to potentially address all components of the neuromuscular associated Pompe disease pathology.

Topics & Concepts

Genetic enhancementEnzyme replacement therapyMedicineDiseaseViral vectorAdeno-associated virusCell therapyBioinformaticsGlycogen storage disease type IIStem-cell therapyVector (molecular biology)ImmunologyStem cellPathologyGeneBiologyMesenchymal stem cellGeneticsRecombinant DNALysosomal Storage Disorders ResearchVirus-based gene therapy researchCytomegalovirus and herpesvirus research