Skip to Content
MilliporeSigma
  • Excess sphingomyelin disturbs ATG9A trafficking and autophagosome closure.

Excess sphingomyelin disturbs ATG9A trafficking and autophagosome closure.

Autophagy (2016-04-14)
Elisabeth Corcelle-Termeau, Signe Diness Vindeløv, Saara Hämälistö, Baharia Mograbi, Anne Keldsbo, Jan Hinrich Bräsen, Elena Favaro, Dieter Adam, Piotr Szyniarowski, Paul Hofman, Stefan Krautwald, Thomas Farkas, Nikolaj H T Petersen, Mikkel Rohde, Andreas Linkermann, Marja Jäättelä
ABSTRACT

Sphingomyelin is an essential cellular lipid that traffics between plasma membrane and intracellular organelles until directed to lysosomes for SMPD1 (sphingomyelin phosphodiesterase 1)-mediated degradation. Inactivating mutations in the SMPD1 gene result in Niemann-Pick diseases type A and B characterized by sphingomyelin accumulation and severely disturbed tissue homeostasis. Here, we report that sphingomyelin overload disturbs the maturation and closure of autophagic membranes. Niemann-Pick type A patient fibroblasts and SMPD1-depleted cancer cells accumulate elongated and unclosed autophagic membranes as well as abnormally swollen autophagosomes in the absence of normal autophagosomes and autolysosomes. The immature autophagic membranes are rich in WIPI2, ATG16L1 and MAP1LC3B but display reduced association with ATG9A. Contrary to its normal trafficking between plasma membrane, intracellular organelles and autophagic membranes, ATG9A concentrates in transferrin receptor-positive juxtanuclear recycling endosomes in SMPD1-deficient cells. Supporting a causative role for ATG9A mistrafficking in the autophagy defect observed in SMPD1-deficient cells, ectopic ATG9A effectively reverts this phenotype. Exogenous C12-sphingomyelin induces a similar juxtanuclear accumulation of ATG9A and subsequent defect in the maturation of autophagic membranes in healthy cells while the main sphingomyelin metabolite, ceramide, fails to revert the autophagy defective phenotype in SMPD1-deficient cells. Juxtanuclear accumulation of ATG9A and defective autophagy are also evident in tissues of smpd1-deficient mice with a subsequent inability to cope with kidney ischemia-reperfusion stress. These data reveal sphingomyelin as an important regulator of ATG9A trafficking and maturation of early autophagic membranes.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
OptiPrep Density Gradient Medium, used for cell and subcellular organelle isolation
Sigma-Aldrich
Periodic Acid-Schiff (PAS) Staining System
Sigma-Aldrich
Monoclonal Anti-Ceramide antibody produced in mouse, clone MID 15B4, purified immunoglobulin, buffered aqueous solution
Sigma-Aldrich
Ethanol, puriss. p.a., absolute, ≥99.8% (GC)
Sigma-Aldrich
Bromophenol Blue, titration: suitable
Sigma-Aldrich
Sphingomyelinase from Bacillus cereus, buffered aqueous glycerol solution, ≥100 units/mg protein (Lowry)
Sigma-Aldrich
Xylenes, histological grade
Sigma-Aldrich
MISSION® esiRNA, targeting human ATG4B