Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress

Hong Peng; Jiao Yang; Guangyi Li; Qing You; Wen Han; Tianrang Li; Daming Gao; Xiaoduo Xie; Byung Hoon Lee; Juan Du; Jian Hou; Tao Zhang; Hai Rao; Ying Huang; Qinrun Li; Rong Zeng; Lijian Hui; Hongyan Wang; Qin Xia; Xuemin Zhang; Yongning He; Masaaki Komatsu; Ivan Dikic; Daniel Finley; Ronggui Hu

doi:10.1038/cr.2017.40

Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress

Hong Peng, Jiao Yang, Guangyi Li, Qing You, Wen Han, Tianrang Li, Daming Gao, Xiaoduo Xie, Byung Hoon Lee, Juan Du, Jian Hou, Tao Zhang, Hai Rao, Ying Huang, Qinrun Li, Rong Zeng, Lijian Hui, Hongyan Wang, Qin Xia, Xuemin ZhangYongning He, Masaaki Komatsu, Ivan Dikic, Daniel Finley, Ronggui Hu^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

137 Citations (Scopus)

Abstract

Alterations in cellular ubiquitin (Ub) homeostasis, known as Ub stress, feature and affect cellular responses in multiple conditions, yet the underlying mechanisms are incompletely understood. Here we report that autophagy receptor p62/sequestosome-1 interacts with E2 Ub conjugating enzymes, UBE2D2 and UBE2D3. Endogenous p62 undergoes E2-dependent ubiquitylation during upregulation of Ub homeostasis, a condition termed as Ub + stress, that is intrinsic to Ub overexpression, heat shock or prolonged proteasomal inhibition by bortezomib, a chemotherapeutic drug. Ubiquitylation of p62 disrupts dimerization of the UBA domain of p62, liberating its ability to recognize polyubiquitylated cargoes for selective autophagy. We further demonstrate that this mechanism might be critical for autophagy activation upon Ub + stress conditions. Delineation of the mechanism and regulatory roles of p62 in sensing Ub stress and controlling selective autophagy could help to understand and modulate cellular responses to a variety of endogenous and environmental challenges, potentially opening a new avenue for the development of therapeutic strategies against autophagy-related maladies.

Original language	English
Pages (from-to)	657-674
Number of pages	18
Journal	Cell Research
Volume	27
Issue number	5
DOIs	https://doi.org/10.1038/cr.2017.40
Publication status	Published - 1 May 2017
Externally published	Yes

Keywords

Autophagy receptor
Dynamic light scattering
Heat shock
Selective autophagy
Ubiquitin
Ubiquitylation

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10.1038/cr.2017.40

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Peng, H., Yang, J., Li, G., You, Q., Han, W., Li, T., Gao, D., Xie, X., Lee, B. H., Du, J., Hou, J., Zhang, T., Rao, H., Huang, Y., Li, Q., Zeng, R., Hui, L., Wang, H., Xia, Q., ... Hu, R. (2017). Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress. Cell Research, 27(5), 657-674. https://doi.org/10.1038/cr.2017.40

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title = "Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress",

abstract = "Alterations in cellular ubiquitin (Ub) homeostasis, known as Ub stress, feature and affect cellular responses in multiple conditions, yet the underlying mechanisms are incompletely understood. Here we report that autophagy receptor p62/sequestosome-1 interacts with E2 Ub conjugating enzymes, UBE2D2 and UBE2D3. Endogenous p62 undergoes E2-dependent ubiquitylation during upregulation of Ub homeostasis, a condition termed as Ub + stress, that is intrinsic to Ub overexpression, heat shock or prolonged proteasomal inhibition by bortezomib, a chemotherapeutic drug. Ubiquitylation of p62 disrupts dimerization of the UBA domain of p62, liberating its ability to recognize polyubiquitylated cargoes for selective autophagy. We further demonstrate that this mechanism might be critical for autophagy activation upon Ub + stress conditions. Delineation of the mechanism and regulatory roles of p62 in sensing Ub stress and controlling selective autophagy could help to understand and modulate cellular responses to a variety of endogenous and environmental challenges, potentially opening a new avenue for the development of therapeutic strategies against autophagy-related maladies.",

keywords = "Autophagy receptor, Dynamic light scattering, Heat shock, Selective autophagy, Ubiquitin, Ubiquitylation",

author = "Hong Peng and Jiao Yang and Guangyi Li and Qing You and Wen Han and Tianrang Li and Daming Gao and Xiaoduo Xie and Lee, {Byung Hoon} and Juan Du and Jian Hou and Tao Zhang and Hai Rao and Ying Huang and Qinrun Li and Rong Zeng and Lijian Hui and Hongyan Wang and Qin Xia and Xuemin Zhang and Yongning He and Masaaki Komatsu and Ivan Dikic and Daniel Finley and Ronggui Hu",

year = "2017",

month = may,

day = "1",

doi = "10.1038/cr.2017.40",

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journal = "Cell Research",

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Peng, H, Yang, J, Li, G, You, Q, Han, W, Li, T, Gao, D, Xie, X, Lee, BH, Du, J, Hou, J, Zhang, T, Rao, H, Huang, Y, Li, Q, Zeng, R, Hui, L, Wang, H, Xia, Q, Zhang, X, He, Y, Komatsu, M, Dikic, I, Finley, D & Hu, R 2017, 'Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress', Cell Research, vol. 27, no. 5, pp. 657-674. https://doi.org/10.1038/cr.2017.40

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T1 - Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress

AU - Peng, Hong

AU - Yang, Jiao

AU - Li, Guangyi

AU - You, Qing

AU - Han, Wen

AU - Li, Tianrang

AU - Gao, Daming

AU - Xie, Xiaoduo

AU - Lee, Byung Hoon

AU - Du, Juan

AU - Hou, Jian

AU - Zhang, Tao

AU - Rao, Hai

AU - Huang, Ying

AU - Li, Qinrun

AU - Zeng, Rong

AU - Hui, Lijian

AU - Wang, Hongyan

AU - Xia, Qin

AU - Zhang, Xuemin

AU - He, Yongning

AU - Komatsu, Masaaki

AU - Dikic, Ivan

AU - Finley, Daniel

AU - Hu, Ronggui

PY - 2017/5/1

Y1 - 2017/5/1

N2 - Alterations in cellular ubiquitin (Ub) homeostasis, known as Ub stress, feature and affect cellular responses in multiple conditions, yet the underlying mechanisms are incompletely understood. Here we report that autophagy receptor p62/sequestosome-1 interacts with E2 Ub conjugating enzymes, UBE2D2 and UBE2D3. Endogenous p62 undergoes E2-dependent ubiquitylation during upregulation of Ub homeostasis, a condition termed as Ub + stress, that is intrinsic to Ub overexpression, heat shock or prolonged proteasomal inhibition by bortezomib, a chemotherapeutic drug. Ubiquitylation of p62 disrupts dimerization of the UBA domain of p62, liberating its ability to recognize polyubiquitylated cargoes for selective autophagy. We further demonstrate that this mechanism might be critical for autophagy activation upon Ub + stress conditions. Delineation of the mechanism and regulatory roles of p62 in sensing Ub stress and controlling selective autophagy could help to understand and modulate cellular responses to a variety of endogenous and environmental challenges, potentially opening a new avenue for the development of therapeutic strategies against autophagy-related maladies.

AB - Alterations in cellular ubiquitin (Ub) homeostasis, known as Ub stress, feature and affect cellular responses in multiple conditions, yet the underlying mechanisms are incompletely understood. Here we report that autophagy receptor p62/sequestosome-1 interacts with E2 Ub conjugating enzymes, UBE2D2 and UBE2D3. Endogenous p62 undergoes E2-dependent ubiquitylation during upregulation of Ub homeostasis, a condition termed as Ub + stress, that is intrinsic to Ub overexpression, heat shock or prolonged proteasomal inhibition by bortezomib, a chemotherapeutic drug. Ubiquitylation of p62 disrupts dimerization of the UBA domain of p62, liberating its ability to recognize polyubiquitylated cargoes for selective autophagy. We further demonstrate that this mechanism might be critical for autophagy activation upon Ub + stress conditions. Delineation of the mechanism and regulatory roles of p62 in sensing Ub stress and controlling selective autophagy could help to understand and modulate cellular responses to a variety of endogenous and environmental challenges, potentially opening a new avenue for the development of therapeutic strategies against autophagy-related maladies.

KW - Autophagy receptor

KW - Dynamic light scattering

KW - Heat shock

KW - Selective autophagy

KW - Ubiquitin

KW - Ubiquitylation

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U2 - 10.1038/cr.2017.40

DO - 10.1038/cr.2017.40

M3 - Article

C2 - 28322253

AN - SCOPUS:85015717176

SN - 1001-0602

VL - 27

SP - 657

EP - 674

JO - Cell Research

JF - Cell Research

IS - 5

ER -

Ubiquitylation of p62/sequestosome1 activates its autophagy receptor function and controls selective autophagy upon ubiquitin stress

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Keywords

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