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Modulating Autophagy as a Treatment for Lysosomal Storage Diseases
Case ID:
TAB-2353
Web Published:
12/6/2022
Researchers at NIAMS have developed a technology for treatment of lysosomal storage diseases by inhibition of autophagy. Pompe disease is an example of a genetic lysosomal storage disease caused by a reduction or absence of acid alpha-glucosidase (GAA). Patients with Pompe disease have a lysosomal buildup of glycogen in cardiac and skeletal muscle cells and severe cardiomyopathy and skeletal muscle myopathy. Treatment of Pompe disease by GAA enzyme replacement therapy is quite ineffective for the skeletal muscle myopathy. Skeletal muscle resistance to therapy is associated with increased cellular buildup of autophagic debris. Inactivation of autophagy results in effective GAA replacement therapy and a reduction in glycogen back to normal levels. This technology provides a novel approach for the treatment of Pompe disease as well as other diseases where autophagy is a critical contributor to disease development.
Patent Information:
Title
App Type
Country
Serial No.
Patent No.
File Date
Issued Date
Expire Date
Direct Link:
https://canberra-ip.technologypublisher.com/tech/Modulating_Autophagy_as_a_Tr eatment_for_Lysosomal_Storage_Diseases
Keywords:
Acid
A-glucosidase
Autophagy
B
Clearance
Complete
DEFICIENCY
Disabling
Disease
Enzyme
ERT
GB1XXX
GBXXXX
Genetic
GLYCOGEN
GXXXXX
IBXXXX
Inactivation
IXXXXX
Lysosomal
Model
Mouse
MUSCLE
Near
Patent Category - Biotechnology
Permits
Pompe
REPLACEMENT
SKELETAL
Storage
STORED
THERAPY
UA1XXX
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For Information, Contact:
Vladimir Knezevic
Senior Advisor for Commercial Evaluations
NIH Technology Transfer
vlado.knezevic@nih.gov