In selective autophagy, cytoplasmic components are selected and tagged before being sequestered into an autophagosome by means of selective autophagy receptors such as p62/SQSTM1. In this review, we discuss how selective autophagy is regulated. An important level of regulation is the selection of proteins or organelles for degradation. Components selected for degradation are tagged, often with ubiquitin, to facilitate recognition by autophagy receptors. Another level of regulation is represented by the autophagy receptors themselves. For p62, its ability to co-aggregate with ubiquitinated substrates is strongly induced by post-translational modifications (PTMs). The transcription of p62 is also markedly increased during conditions in which selective autophagy substrates accumulate. For other autophagy receptors, the LC3-interacting region (LIR) motif is regulated by PTMs, inhibiting or stimulating the interaction with ATG8 family proteins. ATG8 proteins are also regulated by PTMs. Regulation of the capacity of the core autophagy machinery also affects selective autophagy. Importantly, autophagy receptors can induce local recruitment and activation of ULK1/2 and PI3KC3 complexes at the site of cargo sequestration.
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December 2017
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This issue of Essays in Biochemistry covers a range of topics in autophagy signalling, touching on emerging new details on the mechanisms of autophagy regulation, novel aspects of selective autophagy and how autophagy functions in organelle homeostasis. It also looks at how autophagy research is leading to better understanding of human disease and plant biology that can be exploited for the benefit of society. Cover image credit: Kateryna Kon (Shutterstock: 494829457)
Review Article|
December 12 2017
Regulation of selective autophagy: the p62/SQSTM1 paradigm
Trond Lamark;
Trond Lamark
1Molecular Cancer Research Group, Institute of Medical Biology, University of Tromsø– The Arctic University of Norway, Tromsø9037, Norway
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Steingrim Svenning;
Steingrim Svenning
1Molecular Cancer Research Group, Institute of Medical Biology, University of Tromsø– The Arctic University of Norway, Tromsø9037, Norway
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Terje Johansen
1Molecular Cancer Research Group, Institute of Medical Biology, University of Tromsø– The Arctic University of Norway, Tromsø9037, Norway
Correspondence: Terje Johansen (terje.johansen@uit.no)
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Essays Biochem (2017) 61 (6): 609–624.
Article history
Received:
August 31 2017
Revision Received:
October 19 2017
Accepted:
October 19 2017
Citation
Jon D. Lane, Viktor I. Korolchuk, James T. Murray, Trond Lamark, Steingrim Svenning, Terje Johansen; Regulation of selective autophagy: the p62/SQSTM1 paradigm. Essays Biochem 12 December 2017; 61 (6): 609–624. doi: https://doi.org/10.1042/EBC20170035
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