Down syndrome fibroblasts exhibit diminished autophagic clearance and endosomal dysfunction after serum starvation

Abstract: Down syndrome (DS) is a genetic disorder caused by trisomy of chromosome 21 (Tri21). This unbalanced karyotype has the ability to produce proteotoxic stress and dysfunction of the proteostasis network (PN), which are mechanistically associated with several comorbidities found in the DS phenotype. Autophagy is the cellular process responsible for bulk protein degradation and its impairment could negatively impact protein quality control. Based on our previous observations of PN disruption in DS, we investigated… Show more

“…13 ). Diminished autophagic clearance along with lysosomal impairments have been already reported in DS [ [65] , [66] , [67] , [68] ]. However, the novel aspect of the current study is that CBS inhibition normalizes some of these alterations, thereby further promoting the availability of the ATG3 component, possibly to facilitate the formation of functional complexes of the autophagic machinery ( Fig.…”

Role of the cystathionine β-synthase / H2S pathway in the development of cellular metabolic dysfunction and pseudohypoxia in down syndrome

“…13 ). Diminished autophagic clearance along with lysosomal impairments have been already reported in DS [ [65] , [66] , [67] , [68] ]. However, the novel aspect of the current study is that CBS inhibition normalizes some of these alterations, thereby further promoting the availability of the ATG3 component, possibly to facilitate the formation of functional complexes of the autophagic machinery ( Fig.…”

Role of the cystathionine β-synthase / H2S pathway in the development of cellular metabolic dysfunction and pseudohypoxia in down syndrome