| Literature DB >> 23669057 |
Erin J Feeney1, Carmine Spampanato, Rosa Puertollano, Andrea Ballabio, Giancarlo Parenti, Nina Raben.
Abstract
It is hard to find an area of biology in which autophagy is not involved. In fact, the topic extends beyond scientific research to stimulate intellectual exercise and entertainment-autophagy has found its way into a crossword puzzle (Klionsky, 2013). We have found yet another function of autophagy while searching for a better treatment for Pompe disease, a devastating metabolic myopathy resulting from excessive lysosomal glycogen storage. To relieve this glycogen burden, we stimulated lysosomal exocytosis through upregulation of transcription factor EB (TFEB). Overexpression of TFEB in Pompe muscle clears the cells of enlarged lysosomes, reduces glycogen levels, and alleviates autophagic buildup, the major secondary abnormality in Pompe disease. Unexpectedly, the process of exocytosis does not seem to be a purely lysosomal event; vesicles arranged along the plasma membrane are double-labeled with the lysosomal marker LAMP1 and the autophagosomal marker LC3, indicating that TFEB induces the exocytosis of autolysosomes. Furthermore, the effects of TFEB are almost abrogated in autophagy-deficient Pompe mice, suggesting a previously unrecognized role of autophagy in TFEB-mediated cellular clearance.Entities:
Keywords: Pompe disease; TFEB; acid alpha-glucosidase; lysosomal exocytosis; lysosomal storage
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Year: 2013 PMID: 23669057 PMCID: PMC3722326 DOI: 10.4161/auto.24920
Source DB: PubMed Journal: Autophagy ISSN: 1554-8627 Impact factor: 16.016