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SNAP23 regulates BAX-dependent adipocyte programmed cell death independently of canonical macroautophagy.

Citation
Feng, D., et al. “Snap23 Regulates Bax-Dependent Adipocyte Programmed Cell Death Independently Of Canonical Macroautophagy.”. The Journal Of Clinical Investigation, pp. 3941-3956.
Center Albert Einstein College of Medicine
Featured
Author Daorong Feng, Dulguun Amgalan, Rajat Singh, Jianwen Wei, Jennifer Wen, Tszki Peter Wei, Timothy E McGraw, Richard N Kitsis, Jeffrey E Pessin
Keywords Adipose tissue, Apoptosis, Autophagy, Cell Biology, Metabolism
Abstract

The t-SNARE protein SNAP23 conventionally functions as a component of the cellular machinery required for intracellular transport vesicle fusion with target membranes and has been implicated in the regulation of fasting glucose levels, BMI, and type 2 diabetes. Surprisingly, we observed that adipocyte-specific KO of SNAP23 in mice resulted in a temporal development of severe generalized lipodystrophy associated with adipose tissue inflammation, insulin resistance, hyperglycemia, liver steatosis, and early death. This resulted from adipocyte cell death associated with an inhibition of macroautophagy and lysosomal degradation of the proapoptotic regulator BAX, with increased BAX activation. BAX colocalized with LC3-positive autophagic vacuoles and was increased upon treatment with lysosome inhibitors. Moreover, BAX deficiency suppressed the lipodystrophic phenotype in the adipocyte-specific SNAP23-KO mice and prevented cell death. In addition, ATG9 deficiency phenocopied SNAP23 deficiency, whereas ATG7 deficiency had no effect on BAX protein levels, BAX activation, or apoptotic cell death. These data demonstrate a role for SNAP23 in the control of macroautophagy and programmed cell death through an ATG9-dependent, but ATG7-independent, pathway regulating BAX protein levels and BAX activation.

Year of Publication
2018
Journal
The Journal of clinical investigation
Volume
128
Issue
9
Number of Pages
3941-3956
Date Published
12/2018
ISSN Number
1558-8238
DOI
10.1172/JCI99217
Alternate Journal
J. Clin. Invest.
PMID
30102258
PMCID
PMC6118598
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