Characteristics and requirements of basal autophagy in HEK 293 cells

Musiwaro, Patience; Smith, Matthew D.; Manifava, Maria; Walker, Simon; Ktistakis, Nicholas T.

doi:10.4161/auto.25455

Cited by 69 publications

(45 citation statements)

References 49 publications

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“…Recently, CQ was reported to activate autophagy by inhibiting mTOR, which could contribute to the increase in LC3-II accumulation observed. 33 Nevertheless, when considered together with the ConA and colocalisation experiments (below), the data support a role for lysosomes in NGF-induced clearance of cleaved caspase-3.…”

Section: Resultsmentioning

confidence: 69%

Nerve growth factor-mediated inhibition of apoptosis post-caspase activation is due to removal of active caspase-3 in a lysosome-dependent manner

et al. 2014

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Nerve growth factor (NGF) is well characterised as an important pro-survival factor in neuronal cells that can inhibit apoptotic cell death upstream of mitochondrial outer membrane permeabilisation. Here we addressed the question of whether NGF can also protect against apoptosis downstream of caspase activation. NGF treatment promoted a rapid reduction in the level of the p17 subunit of active caspase-3 in PC12 cells that had been induced to undergo apoptosis by various cytotoxins. The mechanism involved TrkA-dependent activation of extracellular signal-regulated kinase (ERK1/2) but not phosphatidylinositol 3-kinase (PI3K)/Akt, and de novo protein synthesis. Involvement of inhibitor of apoptosis proteins (IAPs) and proteasomal degradation were ruled out. In contrast, inhibition of lysosome function using chloroquine and concanamycin A reversed NGF-induced removal of p17. Moreover, in NGF-treated cells, active caspases were found to be localised to lysosomes. The involvement of macroautophagy and chaperone-mediated autophagy were ruled out. Taken together, these findings suggest an anti-apoptotic mechanism by which NGF induces removal of active caspase-3 in a lysosome-dependent manner.

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Section: Resultsmentioning

confidence: 69%

Nerve growth factor-mediated inhibition of apoptosis post-caspase activation is due to removal of active caspase-3 in a lysosome-dependent manner

et al. 2014

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“…Starvation-induced autophagy is severely impaired in Vps34 null mutant or dominant-negative Vps34 overexpressing cells, although some autophagosomes form at a reduced rate [51]. This may be explained by the activity of the class II PI3K, which was suggested to partially compensate for the loss of Vps34 during autophagy in mammalian cells [52, 53]. Similarly, deletion of Drosophila Vps15 or Atg6 results in a block of starvation-induced autophagy [54, 55].…”

Section: Genetic Control Of Autophagy In Drosophilamentioning

confidence: 99%

Autophagy inDrosophila: From Historical Studies to Current Knowledge

Mulakkal

Nagy

Takáts

et al. 2014

BioMed Research International

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The discovery of evolutionarily conserved Atg genes required for autophagy in yeast truly revolutionized this research field and made it possible to carry out functional studies on model organisms. Insects including Drosophila are classical and still popular models to study autophagy, starting from the 1960s. This review aims to summarize past achievements and our current knowledge about the role and regulation of autophagy in Drosophila, with an outlook to yeast and mammals. The basic mechanisms of autophagy in fruit fly cells appear to be quite similar to other eukaryotes, and the role that this lysosomal self-degradation process plays in Drosophila models of various diseases already made it possible to recognize certain aspects of human pathologies. Future studies in this complete animal hold great promise for the better understanding of such processes and may also help finding new research avenues for the treatment of disorders with misregulated autophagy.

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“…Autophagy is important for maintaining basal cellular homeostasis under normal conditions [3]. Under stress conditions, such as cancer, serum deprivation, and oxidative stress, autophagy is activated to adapt to the stress-induced structural remodeling by synthesizing more nutrients and energy, removing intracellular long-lived or misfolded proteins, and eliminating superfluous or damaged organelles and invasive microbes [4].…”

Section: Introductionmentioning

confidence: 99%

Autophagy: A Role in the Apoptosis, Survival, Inflammation, and Development of the Retina

Lin

2018

Ophthalmic Res

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Autophagy is a lysosomal degradation process that maintains cellular homeostasis by removing dysfunctional organelles and unfolded proteins. Increasing evidence has shown that autophagy proteins are involved in retinal physiology and pathology and that defective autophagy contributes to retinal degeneration. In retinal diseases, autophagy plays a dual role: promoting retinal cell survival and death. Autophagy at a normal level helps retinal cells defend themselves against harmful stress; however, excessive autophagy results in retinal deterioration. Both synergistic and antagonistic roles of autophagy and apoptosis in the retina have been reported in the literature. In this review, we summarize the roles of autophagy in the development of the retina and retinal diseases. This review highlights the importance of autophagy in retinal diseases, and targeting autophagy may provide a new therapeutic approach for retinal diseases.

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Characteristics and requirements of basal autophagy in HEK 293 cells

Cited by 69 publications

References 49 publications

Nerve growth factor-mediated inhibition of apoptosis post-caspase activation is due to removal of active caspase-3 in a lysosome-dependent manner

Nerve growth factor-mediated inhibition of apoptosis post-caspase activation is due to removal of active caspase-3 in a lysosome-dependent manner

Autophagy inDrosophila: From Historical Studies to Current Knowledge

Autophagy: A Role in the Apoptosis, Survival, Inflammation, and Development of the Retina

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