• Title of article

    FKBP10 Depletion Enhances Glucocerebrosidase Proteostasis in Gaucher Disease Fibroblasts Original Research Article

  • Author/Authors

    Derrick Sek Tong Ong، نويسنده , , Ya-Juan Wang، نويسنده , , Yun Lei Tan، نويسنده , , John R. Yates III، نويسنده , , Ting-Wei Mu، نويسنده , , Jeffery W. Kelly and Carol V. Robinson، نويسنده ,

  • Issue Information
    ماهنامه با شماره پیاپی سال 2013
  • Pages
    13
  • From page
    403
  • To page
    415
  • Abstract
    Lysosomal storage diseases (LSDs) are often caused by mutations compromising lysosomal enzyme folding in the endoplasmic reticulum (ER), leading to degradation and loss of function. Mass spectrometry analysis of Gaucher fibroblasts treated with mechanistically distinct molecules that increase LSD enzyme folding, trafficking, and function resulted in the identification of nine commonly downregulated and two jointly upregulated proteins, which we hypothesized would be critical proteostasis network components for ameliorating loss-of-function diseases. LIMP-2 and FK506 binding protein 10 (FKBP10) were validated as such herein. Increased FKBP10 levels accelerated mutant glucocerebrosidase degradation over folding and trafficking, whereas decreased ER FKBP10 concentration led to more LSD enzyme partitioning into the calnexin profolding pathway, enhancing folding and activity to levels thought to ameliorate LSDs. Thus, targeting FKBP10 appears to be a heretofore unrecognized therapeutic strategy to ameliorate LSDs.
  • Journal title
    Chemistry and Biology
  • Serial Year
    2013
  • Journal title
    Chemistry and Biology
  • Record number

    1160412