Litcius/Paper detail

FAIM regulates autophagy through glutaminolysis in lung adenocarcinoma

Tianyu Han, Pengcheng Wang, Yanan Wang, Wenze Xun, Jiapeng Lei, Tao Wang, Zhuo Lü, Mingxi Gan, Wei Zhang, Bentong Yu, Jianbin Wang

2021Autophagy21 citationsDOIOpen Access PDF

Abstract

Altered glutamine metabolism is an important aspect of cancer metabolic reprogramming. The GLS isoform GAC (glutaminase C), the rate-limiting enzyme in glutaminolysis, plays a vital role in cancer initiation and progression. Our previous studies demonstrated that phosphorylation of GAC was essential for its high enzymatic activity. However, the molecular mechanisms for GAC in maintaining its high enzymatic activity and protein stability still need to be further clarified. FAIM/FAIM1 (Fas apoptotic inhibitory molecule) is known as an important anti-apoptotic protein, but little is known about its function in tumorigenesis. Here, we found that knocking down FAIM induced macroautophagy/autophagy through suppressing the activation of the MTOR pathway in lung adenocarcinoma. Further studies demonstrated that FAIM could promote the tetramer formation of GAC through increasing PRKCE/PKCε-mediated phosphorylation. What's more, FAIM also stabilized GAC through sequestering GAC from degradation by protease ClpXP. These effects increased the production of α-ketoglutarate, leading to the activation of MTOR. Besides, FAIM also promoted the association of ULK1 and MTOR and this further suppressed autophagy induction. These findings discovered new functions of FAIM and elucidated an important molecular mechanism for GAC in maintaining its high enzymatic activity and protein stability.

Topics & Concepts

AutophagyGlutaminolysisBiologyPI3K/AKT/mTOR pathwayCell biologyPhosphorylationGlutaminaseBiochemistrySignal transductionEnzymeGlycolysisApoptosisGlutamineAmino acidAutophagy in Disease and TherapyCancer, Hypoxia, and MetabolismCancer Research and Treatments