Interestingly, at this early stage it is not uncommon to find small damaged lysosomes inside the autophagosome. In an unusual role reversal it appears that
the autophagosome engulfs the lysosome. Since one of the functions of autophagy is the elimination of damaged organelles, it is possible that the presence of damaged lysosomes triggers the increase in autophagy. If this hypothesis is true, the damage to the Inhibitors,research,lifescience,medical lysosomes may occur very early when the lysosomes are still small. As the disease progresses, the autophagic buildup appears to interrupt muscle striation, as demonstrated by immunostaining of single muscle fibers for myosin, a structural muscle protein. There is also an indication of oxidative
stress as evidenced by progressive Inhibitors,research,lifescience,medical accumulation of lipofuscin in muscle fibers, even from young animals. Autofluorescent material in the KO myofibers is concentrated nearly exclusively in the autophagic areas. Enhanced deposition of lipofuscin and large areas of centrally located Inhibitors,research,lifescience,medical cellular debris were observed in muscle biopsies of another mouse model of Pompe disease (16). Lipofuscin, an autofluorescent material composed of oxidatively modified macromolecules, normally accumulates in lysosomes of postmitotic cells ABT-199 in vivo during aging, but abnormal increase of lipofuscin was shown to be associated with oxidative damage (17). The autophagic buildup grows with age, and seems to have a greater effect on muscle architecture than the expanded lysosomes outside the area. As mentioned above, autophagic areas contain multiple vesicular structures in fibers from younger Inhibitors,research,lifescience,medical mice. In contrast,
in old mice (beyond 20 months of age) the integrity of the vesicles in the autophagic areas appears lost and only remnants Inhibitors,research,lifescience,medical of vacuolar membranes can be visualized. This stage most likely represents the point of no return because so little Phosphatidylinositol diacylglycerol-lyase of the muscle structure is intact. Furthermore, at this stage, the autophagic areas are totally devoid of the mannose 6-phosphate receptor, making the delivery of the therapeutic enzyme impossible (11). The relevance of the studies in a murine model of the disease is underscored by the presence of increased autophagy in muscle fibers from patients with Pompe disease. In humans we see many of the same things that were observed in mice. Autophagy appears to be a big player in the pathogenesis of the disease. The autophagic areas which begin at multiple points along the fiber eventually expand, come together, and totally replace muscle tissue. In some fibers, the expanded lysosomes outside the area of autophagy look like innocent bystanders (18).