Biomolecular condensates in autophagy regulation

被引:30
作者
Fujioka, Yuko [1 ]
Noda, Nobuo N. [1 ]
机构
[1] Inst Microbial Chem, Shinagawa Ku, 3-14-23 Kamiosaki, Tokyo 1410021, Japan
来源
CURRENT OPINION IN CELL BIOLOGY | 2021年 / 69卷
关键词
Autophagy; PAS; Ape1; p62; Phase separation; Biomolecular condensate; Selective autophagy; Bulk autophagy; Cvt pathway; SELECTIVE AUTOPHAGY; AMINOPEPTIDASE-I; STRUCTURAL BASIS; ATG1; KINASE; EARLY STEPS; PROTEIN; CYTOPLASM; RECEPTOR; P62; TOR;
D O I
10.1016/j.ceb.2020.12.011
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Autophagy is an intracellular degradation system that contributes to cellular homeostasis. Autophagosome formation is a landmark event in autophagy, which sequesters and delivers cytoplasmic components to the lysosome for degradation. Based on selectivity, autophagy can be classified into bulk and selective autophagy, which are mechanistically distinct from each other, especially in the requirement of cargos for autophagosome formation. Recent studies revealed that liquid-like biomolecular condensates, which are formed through liquid-liquid phase separation, regulate the autophagosome formation of both bulk and selective autophagy. Here, we focus on recent findings on the involvement of biomolecular condensates in autophagy regulation and discuss their significance.
引用
收藏
页码:23 / 29
页数:7
相关论文
共 53 条
[1]   Biomolecular condensates: organizers of cellular biochemistry [J].
Banani, Salman F. ;
Lee, Hyun O. ;
Hyman, Anthony A. ;
Rosen, Michael K. .
NATURE REVIEWS MOLECULAR CELL BIOLOGY, 2017, 18 (05) :285-298
[2]   p62/SQSTM1 forms protein aggregates degraded by autophagy and has a protective effect on huntingtin-induced cell death [J].
Bjorkoy, G ;
Lamark, T ;
Brech, A ;
Outzen, H ;
Perander, M ;
Overvatn, A ;
Stenmark, H ;
Johansen, T .
JOURNAL OF CELL BIOLOGY, 2005, 171 (04) :603-614
[3]   Eukaryotic Stress Granules Are Cleared by Autophagy and Cdc48/VCP Function [J].
Buchan, J. Ross ;
Kolaitis, Regina-Maria ;
Taylor, J. Paul ;
Parker, Roy .
CELL, 2013, 153 (07) :1461-1474
[4]   p62-Dependent Phase Separation of Patient-Derived KEAP1 Mutations and NRF2 [J].
Cloer, E. W. ;
Siesser, P. F. ;
Cousins, E. M. ;
Goldfar, D. ;
Mowrey, D. D. ;
Harrison, J. S. ;
Weir, S. J. ;
Dokholyan, N. V. ;
Major, M. B. .
MOLECULAR AND CELLULAR BIOLOGY, 2018, 38 (22)
[5]   Phase separation organizes the site of autophagosome formation [J].
Fujioka, Yuko ;
Alam, Jahangir Md. ;
Noshiro, Daisuke ;
Mouri, Kazunari ;
Ando, Toshio ;
Okada, Yasushi ;
May, Alexander I. ;
Knorr, Roland L. ;
Suzuki, Kuninori ;
Ohsumi, Yoshinori ;
Noda, Nobuo N. .
NATURE, 2020, 578 (7794) :301-+
[6]   Structural basis of starvation-induced assembly of the autophagy initiation complex [J].
Fujioka, Yuko ;
Suzuki, Sho W. ;
Yamamoto, Hayashi ;
Kondo-Kakuta, Chika ;
Kimura, Yayoi ;
Hirano, Hisashi ;
Akada, Rinji ;
Inagaki, Fuyuhiko ;
Ohsumi, Yoshinori ;
Noda, Nobuo N. .
NATURE STRUCTURAL & MOLECULAR BIOLOGY, 2014, 21 (06) :513-521
[7]   Vac8 determines phagophore assembly site vacuolar localization during nitrogen starvation-induced autophagy [J].
Gatica, Damian ;
Wen, Xin ;
Cheong, Heesun ;
Klionsky, Daniel J. .
AUTOPHAGY, 2021, 17 (07) :1636-1648
[8]   The carboxy terminus of yeast Atg13 binds phospholipid membrane via motifs that overlap with the Vac8-interacting domain [J].
Gatica, Damian ;
Damasio, Alejandro ;
Pascual, Clarence ;
Klionsky, Daniel J. ;
Ragusa, Michael J. ;
Popelka, Hana .
AUTOPHAGY, 2020, 16 (06) :1007-1020
[9]   ER exit sites are physical and functional core autophagosome biogenesis components [J].
Graef, Martin ;
Friedman, Jonathan R. ;
Graham, Christopher ;
Babu, Mohan ;
Nunnari, Jodi .
MOLECULAR BIOLOGY OF THE CELL, 2013, 24 (18) :2918-2931
[10]   Vac8 spatially confines autophagosome formation at the vacuole in S. cerevisiae [J].
Hollenstein, David M. ;
Gomez-Sanchez, Rubeprimen ;
Ciftci, Akif ;
Kriegenburg, Franziska ;
Mari, Muriel ;
Torggler, Raffaela ;
Licheva, Mariya ;
Reggiori, Fulvio ;
Kraft, Claudine .
JOURNAL OF CELL SCIENCE, 2019, 132 (22)
123456