Neuronal Apoptosis Induced by Endoplasmic Reticulum Stress Is Regulated by ATF4–CHOP-Mediated Induction of the Bcl-2 Homology 3-Only Member PUMA

Galehdar, Zohreh; Swan, Patrick; Fuerth, Benjamin J.; Callaghan, Steven M.; Park, David; Cregan, Sean P.

doi:10.1523/jneurosci.1598-10.2010

Cited by 288 publications

(233 citation statements)

References 77 publications

(81 reference statements)

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“…We found that the expression of FADD, caspase-8 and CHOP was not detected in the ischemic core but were obvious in the peri-infarct area, which may be due to the rapid initiation of necrosis in the ischemic core. Moreover, we observed that the ER stressassociated factors were predominantly expressed in the ischemic penumbra, which is in agreement with previous reports that under severe ER stress, apoptotic pathways can be activated inducing the expression of downstream effectors [36][37][38]. Our findings further revealed that T10 significantly down-regulated the expression levels of FADD, caspase-8, and CHOP in the peri-infarct area.…”

Section: Discussionsupporting

confidence: 92%

Triptolide Protects Neurons from Endoplasmic Reticulum Stress-Mediated Apoptosis in Cerebral Ischemic Injury Rats

Su¹,

Zhang²,

Ma³

2016

J Neuroinfect Dis

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This study aimed to investigate the neuroprotective effect of Triptolide (T10) on cerebral ischemia/reperfusion (I/R) injury and explore the underlying mechanisms. Adult male Sprague-Dawley rats were treated with T10 and subjected to middle cerebral artery occlusion (MCAO) for 90 min. Neurological deficits and infarct volume were measured 24 h after reperfusion. ER stress-mediated proteins, ryanodine receptors (RyRs), cysteinyl aspartate specific proteinase 8 (Caspase-8), Fas-associated death domain (FADD) and C/EBP homologous protein (CHOP) were evaluated 1, 4, and 24 h after reperfusion. Pretreatment with 1 mg/kg of T10 significantly reduced infarct volume and neurological deficits. Further, TUNEL staining demonstrated T10 significantly decreased neuronal apoptosis in the peri-infarct area after reperfusion. More importantly, T10 prevented ER stress-mediated expression of RyR, FADD, caspase-8 and CHOP in the peri-infarct area of rats. These results indicate that T10 attenuates the ER stress-induced apoptosis in cerebral I/R injury and suggest that T10 is a promising agent for the treatment of ischemic stroke.

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Section: Discussionsupporting

confidence: 92%

Triptolide Protects Neurons from Endoplasmic Reticulum Stress-Mediated Apoptosis in Cerebral Ischemic Injury Rats

Su¹,

Zhang²,

Ma³

2016

J Neuroinfect Dis

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“…[19][20][21] CHOP can trigger the downregulation of pro-survival BCL2 and upregulation of pro-apoptotic BH3-only proteins BIM 22,23 or PUMA. 20 Additionally, a recent study proposed that increased protein synthesis driven by ATF4/CHOP after re-initiation of general translation increases the amount of reactive oxygen species, thus leading to apoptosis. 13 Therefore, a slower increase in ATF4 levels could be protective.…”

Section: Discussionmentioning

confidence: 99%

Imaging of single cell responses to ER stress indicates that the relative dynamics of IRE1/XBP1 and PERK/ATF4 signalling rather than a switch between signalling branches determine cell survival

et al. 2015

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An accumulation of misfolded proteins in the endoplasmic reticulum (ER) triggers the unfolded protein response (UPR) mediated via the activation of three transmembrane proteins IRE1, PERK and ATF6. Signalling through these proteins is aimed at enhancing the ER folding capacity and reducing the folding load. If these processes fail to re-establish protein homeostasis within the ER, then cell death prevails via apoptosis. How the shift from pro-survival to pro-apoptotic signalling is regulated remains unclear with both IRE1 and PERK signalling associated with pro-survival as well as pro-apoptotic signalling. To investigate the temporal activation of IRE1 and PERK in live cells and their relationship to cellular fate, we devised single cell reporters for both ER stress signalling branches. SH-SY5Y neural cells stably expressing these fluorescent protein reporter constructs to monitor IRE1-splicing activity and PERK-mediated ATF4-translation were imaged using single cell and high content time lapse live cell microscopy. We could correlate an early onset and attenuation of XBP1 splicing in the IRE1-reporter cells as cytoprotective. Indeed, silencing of IRE1 expression using shRNA inhibited splicing of XBP1 resulting in an early onset of cell death. In contrast, in the PERK-reporter cells, we observed that a slow rate of ATF4-translation and late re-initiation of general translation coincided with cells which were resistant to ER stress-induced cell death. Interestingly, whereas silencing of PERK did not affect overall levels of cell death in response to ER stress, it did increase sensitivity to ER stressors at early time points following treatment. Our results suggest that apoptosis activation in response to ER stress is not caused by a preferential activation of a single UPR branch, or by a switch from one branch to the other. Rather, our data indicated that the relative timing of IRE1 and PERK signalling determines the shift from cell survival to apoptosis.

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“…Although the expression of the V37E Cx30 mutant did not induce the upregulation of GRP78, which might occur upon the activation of the activating transcription factor 6 (ATF6) pathway (Berridge, 2002), the V37E mutant only moderately induced the expression of ATF4. ATF4 activates cell-deathinitiating caspases, including caspase 3, through the mitochondria-dependent intrinsic cell death pathway (Galehdar et al, 2010;Groenendyk and Michalak, 2005;Malhotra and Kaufman, 2007). By contrast, the ER-stress-induced splicing of XBP1 through activation of IRE1 did not occur in cells that expressed the V37E mutant, suggesting that the mechanism of cell death might be independent of the UPR.…”

Section: The Loss-of-function V37e Mutant Linked To Clouston and Kidmentioning

confidence: 99%

Mutations in Cx30 that are linked to skin disease and non-syndromic hearing loss exhibit several distinct cellular pathologies

Berger

Kelly

Lajoie

et al. 2014

Journal of Cell Science

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Connexin 30 (Cx30), a member of the large gap junction protein family, plays a role in the homeostasis of the epidermis and inner ear through gap junctional intercellular communication (GJIC). Here, we investigated the underlying mechanisms of four autosomal dominant Cx30 gene mutations linked to hearing loss and/or various skin diseases. First, the T5M mutant linked to non-syndromic hearing loss formed functional gap junction channels and hemichannels, similar to wild type Cx30. The loss-of-function V37E mutant associated with Clouston syndrome or keratitis-ichthyosis-deafness syndrome was retained in the endoplasmic reticulum and significantly induced apoptosis. The G59R mutant linked to Vohwinkel and Bart-Pumphrey syndromes was retained primarily in the Golgi apparatus and exhibited loss of gap junction channel and hemichannel function, but did not cause cell death. Lastly, the A88V mutant related to Clouston syndrome also significantly induced apoptosis, although through an endoplasmic reticulum-independent mechanism. Collectively, we discovered that four unique Cx30 mutants may cause disease through different mechanisms that also likely include their selective transdominant effects on co-expressed connexins, highlighting the overall complexity of connexin-linked diseases and the importance of GJIC in disease prevention.

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Neuronal Apoptosis Induced by Endoplasmic Reticulum Stress Is Regulated by ATF4–CHOP-Mediated Induction of the Bcl-2 Homology 3-Only Member PUMA

Cited by 288 publications

References 77 publications

Triptolide Protects Neurons from Endoplasmic Reticulum Stress-Mediated Apoptosis in Cerebral Ischemic Injury Rats

Triptolide Protects Neurons from Endoplasmic Reticulum Stress-Mediated Apoptosis in Cerebral Ischemic Injury Rats

Imaging of single cell responses to ER stress indicates that the relative dynamics of IRE1/XBP1 and PERK/ATF4 signalling rather than a switch between signalling branches determine cell survival

Mutations in Cx30 that are linked to skin disease and non-syndromic hearing loss exhibit several distinct cellular pathologies

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