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Molecular machinery of macroautophagy and its deregulation in diseases

Journal

BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR BASIS OF DISEASE
Volume 1812, Issue 11, Pages 1490-1497

Publisher

ELSEVIER
DOI: 10.1016/j.bbadis.2011.07.005

Keywords

Autophagy; Autophagosome; Cdk5; Endophilin B1; Post-translational modification; Neurodegenerative disorder

Funding

  1. Research Grants Council of Hong Kong [HKUST 661007, 661109, 660309, 660210, 6/CRF/08]
  2. University Grants Committee [AoE/B-15/01]
  3. Hong Kong Jockey Club
  4. Croucher Foundation

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Macroautophagy maintains cellular homeostasis through targeting cytoplasmic contents and organelles into autophagosomes for degradation. This process begins with the assembly of protein complexes on isolation membrane to initiate the formation of autophagosome, followed by its nucleation, elongation and maturation. Fusion of autophagosomes with lysosomes then leads to degradation of the cargo. In the past decade, significant advances have been made on the identification of molecular players that are implicated in various stages of macroautophagy. Post-translational modifications of macroautophagy regulators have also been demonstrated to be critical for the selective targeting of cytoplasmic contents into autophagosomes. In addition, recent demonstration of distinct macroautophagy regulators has led to the identification of different subtypes of macroautophagy. Since deregulation of macroautophagy is implicated in diseases including neurodegenerative disorders, cancers and inflammatory disorders, understanding the molecular machinery of macroautophagy is crucial for elucidating the mechanisms by which macroautophagy is deregulated in these diseases, thereby revealing new potential therapeutic targets and strategies. Here we summarize current knowledge on the regulation of mammalian macroautophagy machineries and their disease-associated deregulation. (C) 2011 Elsevier B.V. All rights reserved.

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