Development of LC3/GABARAP sensors containing a LIR and a hydrophobic domain to monitor autophagy

You Kyung Lee, Yong Woo Jun, Ha Eun Choi, Yang Hoon Huh, Bong Kiun Kaang, Deok Jin Jang, Jin A. Lee

Research output: Contribution to journalArticlepeer-review

52 Scopus citations

Abstract

Macroautophagy allows for bulk degradation of cytosolic components in lysosomes. Overexpression of GFP/RFP-LC3/GABARAP is commonly used to monitor autophagosomes, a hallmark of autophagy, despite artifacts related to their overexpression. Here, we developed new sensors that detect endogenous LC3/GABARAP proteins at the autophagosome using an LC3-interacting region (LIR) and a short hydrophobic domain (HyD). Among HyD-LIR-GFP sensors harboring LIR motifs of 34 known LC3-binding proteins, HyD-LIR(TP)-GFP using the LIR motif from TP53INP2 allowed detection of all LC3/GABARAPs-positive autophagosomes. However, HyD-LIR(TP)-GFP preferentially localized to GABARAP/GABARAPL1-positive autophagosomes in a LIR-dependent manner. In contrast, HyD-LIR(Fy)-GFP using the LIR motif from FYCO1 specifically detected LC3A/B-positive autophagosomes. HyD-LIR(TP)-GFP and HyD-LIR(Fy)-GFP efficiently localized to autophagosomes in the presence of endogenous LC3/GABARAP levels and without affecting autophagic flux. Both sensors also efficiently localized to MitoTracker-positive damaged mitochondria upon mitophagy induction. HyD-LIR(TP)-GFP allowed live-imaging of dynamic autophagosomes upon autophagy induction. These novel autophagosome sensors can thus be widely used in autophagy research.

Original languageEnglish
Pages (from-to)1100-1116
Number of pages17
JournalEMBO Journal
Volume36
Issue number8
DOIs
StatePublished - 13 Apr 2017

Keywords

  • LC3-interacting region motif
  • autophagosome sensor
  • autophagy
  • hydrophobic domain

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