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Article Abstract
Saposin C deficiency, a rare variant form of Gaucher disease, is due to mutations in the prosaposin gene (PSAP) affecting saposin C expression and/or function. We previously reported that saposin C mutations affecting one cysteine residue result in autophagy dysfunction. We further demonstrated that the accumulation of autophagosomes, observed in saposin C-deficient fibroblasts, is due to an impairment of autolysosome degradation, partially caused by the reduced amount and enzymatic activity of CTSB (cathepsin B) and CTSD (cathepsin D). The restoration of both proteases in pathological fibroblasts results in almost completely recovery of autophagic flux and lysosome homeostasis.
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| http://dx.doi.org/10.4161/auto.22557 | DOI Listing |
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Article Synopsis
- * Deficiencies in GCase activity lead to Gaucher Disease (GD) and can arise from mutations in the GCase-encoding gene, or rarely, from deficiencies in SapC or LIMP-2, which are responsible for targeting GCase to lysosomes.
- * The study reports new cases of LIMP-2 and SapC deficiencies, analyzing the effects on GCase activity and identifying distinct biochemical profiles and degradation pathways in different deficiency types compared to typical G
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