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Open AccessJournal ArticleDOI

The machinery of macroautophagy

Yuchen Feng, +3 more
- 01 Jan 2014 - 
- Vol. 24, Iss: 1, pp 24-41
TLDR
This review focuses on macroautophagy, briefly describing the discovery of this process in mammalian cells, discussing the current views concerning the donor membrane that forms the phagophore, and characterizing the autophagy machinery including the available structural information.
Abstract
Autophagy is a primarily degradative pathway that takes place in all eukaryotic cells. It is used for recycling cytoplasm to generate macromolecular building blocks and energy under stress conditions, to remove superfluous and damaged organelles to adapt to changing nutrient conditions and to maintain cellular homeostasis. In addition, autophagy plays a critical role in cytoprotection by preventing the accumulation of toxic proteins and through its action in various aspects of immunity including the elimination of invasive microbes and its participation in antigen presentation. The most prevalent form of autophagy is macroautophagy, and during this process, the cell forms a double-membrane sequestering compartment termed the phagophore, which matures into an autophagosome. Following delivery to the vacuole or lysosome, the cargo is degraded and the resulting macromolecules are released back into the cytosol for reuse. The past two decades have resulted in a tremendous increase with regard to the molecular studies of autophagy being carried out in yeast and other eukaryotes. Part of the surge in interest in this topic is due to the connection of autophagy with a wide range of human pathophysiologies including cancer, myopathies, diabetes and neurodegenerative disease. However, there are still many aspects of autophagy that remain unclear, including the process of phagophore formation, the regulatory mechanisms that control its induction and the function of most of the autophagy-related proteins. In this review, we focus on macroautophagy, briefly describing the discovery of this process in mammalian cells, discussing the current views concerning the donor membrane that forms the phagophore, and characterizing the autophagy machinery including the available structural information.

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Citations
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Journal ArticleDOI

Targeting autophagy in cancer

TL;DR: A way forward is suggested for the effective targeting of autophagy by understanding the context-dependent roles of autophile and by capitalizing on modern approaches to clinical trial design.
Journal ArticleDOI

Cargo recognition and degradation by selective autophagy

TL;DR: Different types of selective autophagy are discussed, emphasizing the role of ligand receptors and scaffold proteins in providing cargo specificity, and unanswered questions in the field are highlighted.
Journal ArticleDOI

Targeting autophagy in cancer

TL;DR: Fundamental advances in the biology of autophagy are presented, approaches to targeting Autophagy, the preclinical rationale and clinical experience with hydroxychloroquine in cancer clinical trials, the potential role ofAutophagy in tumor immunity, and recent developments in next‐generation autophagic inhibitors that have clinical potential are presented.
Journal ArticleDOI

Autophagy and Tumor Metabolism

TL;DR: The diverse metabolic fuel sources that can be produced by autophagy provide tumors with metabolic plasticity and can allow them to thrive in what can be an austere microenvironment, and understanding how autophile can fuel cellular metabolism will enable more effective combinatorial therapeutic strategies.
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Cellular adaptation to hypoxia through hypoxia inducible factors and beyond.

TL;DR: Understanding these processes could shed light on pathologies associated with hypoxia, including cardiovascular diseases and cancer, and disease mechanisms, such as inflammation and wound repair.
References
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Journal ArticleDOI

Noncanonical E2 recruitment by the autophagy E1 revealed by Atg7–Atg3 and Atg7–Atg10 structures

TL;DR: The data suggest that common principles underlie conjugation in both noncanonical and canonical UBL cascades, whereby flexibly tethered E1 domains recruit E2s through surfaces remote from their active sites to juxtapose the E1 and E2 catalytic cysteines.
Journal ArticleDOI

Defective quality control mechanisms and accumulation of damaged mitochondria link Gaucher and Parkinson diseases

TL;DR: Observations show that dysfunction of cellular quality control pathways lead to impaired energy and free radical homeostasis in GD, providing new insights into the mechanisms of neurodegeneration in GD and illuminating the links between GD and PD.
Journal ArticleDOI

Peroxisome size provides insights into the function of autophagy-related proteins.

TL;DR: A yeast model system is developed to study the effect of cargo size on the requirement of autophagy-related (Atg) proteins and found that peroxisome size determines the requirements of Atg11 and Atg26, suggesting it is a component of the core autophagic machinery.
Journal ArticleDOI

Glycogen autophagosomes in polymorphonuclear leukocytes induced by rickettsiae

TL;DR: Results suggest that rickettisae induce the rapid formation of glycogen‐containing autophagosomes in guinea pig peritoneal PMNs in vitro.
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