Autophagy Is Activated for Cell Survival after Endoplasmic ReticulumStress

Ogata, Maiko; Hino, Shin Ichiro; Saito, Atsushi; Morikawa, Keisuke; Kondo, Shinichi; Kanemoto, Soshi; Murakami, Tomohiko; Taniguchi, Manabu; Tanii, Ichiro; Yoshinaga, Kazuya; Shiosaka, Sadao; Hammarback, James A.; Urano, Fumihiko; Imaizumi, Kazunori

doi:10.1128/mcb.01453-06

Cited by 1,628 publications

(1,500 citation statements)

References 49 publications

(38 reference statements)

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“…When treated with ER stress, atg5 À/À cells died faster than atg5 þ / þ cells (Supplementary Figure S5D), consistent with recent reports that autophagy acts as a survival mechanism to suppress apoptosis in response to ER stress. 16,17 As anticipated, Bcl-xL protected both atg5 þ / þ and atg5 À/À cells from acute apoptosis. In response to prolonged ER stress the Bcl-xLoverexpressing cells progressively died.…”

supporting

confidence: 71%

“…[16][17][18][19] In contrast, in apoptosis-deficient cells prolonged autophagy provokes cell death, and its absence imparts protection. This may be because in these cells where excessive ER stress fails to induce apoptosis, the stressing situation keeps accumulating to a point where autophagy is massively induced subsequently leading to cell damage and necrosis.…”

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confidence: 99%

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Autophagy promotes necrosis in apoptosis-deficient cells in response to ER stress

et al. 2007

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supporting

confidence: 71%

mentioning

confidence: 99%

Autophagy promotes necrosis in apoptosis-deficient cells in response to ER stress

et al. 2007

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“…Studies reported that ER stress led to autophagy [30][31][32] and that RINT1 was associated with autophagy. 21 Therefore, we decided to monitor autophagy in Rint1-deficient cortices.…”

Section: Resultsmentioning

confidence: 99%

Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain

et al. 2015

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Endoplasmic reticulum (ER) stress, defective autophagy and genomic instability in the central nervous system are often associated with severe developmental defects and neurodegeneration. Here, we reveal the role played by Rint1 in these different biological pathways to ensure normal development of the central nervous system and to prevent neurodegeneration. We found that inactivation of Rint1 in neuroprogenitors led to death at birth. Depletion of Rint1 caused genomic instability due to chromosome fusion in dividing cells. Furthermore, Rint1 deletion in developing brain promotes the disruption of ER and Cis/Trans Golgi homeostasis in neurons, followed by ER-stress increase. Interestingly, Rint1 deficiency was also associated with the inhibition of the autophagosome clearance. Altogether, our findings highlight the crucial roles of Rint1 in vivo in genomic stability maintenance, as well as in prevention of ER stress and autophagy.

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“…These vesicles, termed autophagosomes, then fuse to lysosomes, forming autolysosomes, which break down the contents of the vesicle (Figure 1.4). Autophagy can be induced under a range of situations and stimuli, including growth factor withdrawal 114 , inhibition of degradation by the ubiquitin-proteasome system 115 , increases in cytosolic calcium 116 and endoplasmic reticulum stress 117 . Morphologically, autophagy can be identified by electron microscopy where cytoplasmic vacuolation without chromatin condensation is observed.…”

Section: Autophagymentioning

confidence: 99%

Role of the pro-survival molecule Bfl-1 in melanoma

Hind

Carter

Harris

et al. 2015

The International Journal of Biochemistry & Cell Biology

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Melanoma, the cancer derived from the melanocytes of the skin, is becoming an ever more common cancer in the ageing population of the developed world and displays an intrinsic resistance to current therapies. This chemo resistance makes metastatic melanoma an extremely difficult cancer to treat leading to a 5 year survival rate of just 20%. As such, it is important to unearth new potential drug targets to increase the prospects for melanoma patients.Bfl-1 is a pro-survival protein of the Bcl-2 family of apoptosis regulating proteins. It has been found to be over-expressed in a small subset of chemo resistant tumours, including melanoma. Accordingly, I characterised the molecule in melanoma cells and determined its role in protecting these cells from chemotherapy-induced apoptosis. I elucidated the expression profile and half-lives of the protein and mRNA across a panel of melanoma cell-lines and healthy melanocytes. I also confirmed, using pathway specific inhibitors, that Bfl-1 was transcriptionally regulated by the NFB pathway and concluded through pulsechase experiments that Bfl-1 protein was degraded, at least in part, by the proteasome. Subcellular fractionation and indirect immunofluorescence techniques elucidated that Bfl-1 was located mostly at the mitochondria in both resting and apoptotic cells, with a diffuse level present throughout the cytoplasm. As well as characterising the protein in both melanoma cells and healthy primary melanocytes, I determined its role in the resistance of these cells to apoptosis. Over-expressed Bfl-1 was found to protect melanoma cells from apoptosis caused by a range of chemotherapeutic agents in A375 melanoma cells, which naturally expressed very low levels of Bfl-1. Further, knock down of Bfl-1 using siRNA technology in melanoma cells revealed the dependence of these cells on Bfl-1 for their resistance to certain chemotherapeutic agents currently used in melanoma treatment, including the MEK inhibitor PD901. All together, this research contributes to our understanding of Bfl-1 and highlights it as a potentially important therapeutic target in metastatic melanoma.

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Autophagy Is Activated for Cell Survival after Endoplasmic ReticulumStress

Cited by 1,628 publications

References 49 publications

Autophagy promotes necrosis in apoptosis-deficient cells in response to ER stress

Autophagy promotes necrosis in apoptosis-deficient cells in response to ER stress

Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain

Role of the pro-survival molecule Bfl-1 in melanoma

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