Your search keyword '"EIF-2 kinase"' showing total 56 results

1. Genetic Variations in EIF2AK3 are Associated with Neurocognitive Impairment in People Living with HIV.

Author

Akay-Espinoza, Cagla, Akay-Espinoza, Cagla, Newton, Sarah, Dombroski, Beth, Kallianpur, Asha, Bharti, Ajay, Franklin, Donald, Schellenberg, Gerard, Heaton, Robert, Grant, Igor, Ellis, Ronald, Letendre, Scott, Jordan-Sciutto, Kelly, Akay-Espinoza, Cagla, Akay-Espinoza, Cagla, Newton, Sarah, Dombroski, Beth, Kallianpur, Asha, Bharti, Ajay, Franklin, Donald, Schellenberg, Gerard, Heaton, Robert, Grant, Igor, Ellis, Ronald, Letendre, Scott, and Jordan-Sciutto, Kelly

Abstract

Based on emerging evidence on the role for specific single-nucleotide variants (SNVs) in EIF2AK3 encoding the integrated stress response kinase PERK, in neurodegeneration, we assessed the association of EIF2AK3 SNVs with neurocognitive performance in people with HIV (PWH) using a candidate gene approach. This retrospective study included the CHARTER cohort participants, excluding those with severe neuropsychiatric comorbidities. Genome-wide data previously obtained for 1047 participants and targeted sequencing of 992 participants with available genomic DNA were utilized to interrogate the association of three noncoding and three coding EIF2AK3 SNVs with the continuous global deficit score (GDS) and global neurocognitive impairment (NCI; GDS ≥ 0.5) using univariable and multivariable methods, with demographic, disease-associated, and treatment characteristics as covariates. The cohort characteristics were as follows: median age, 43.1 years; females, 22.8%; European ancestry, 41%; median CD4 + T cell counts, 175/µL (nadir) and 428/µL (current). At first assessment, 70.5% used ART and 68.3% of these had plasma HIV RNA levels ≤ 200 copies/mL. All three noncoding EIF2AK3 SNVs were associated with GDS and NCI (all p < 0.05). Additionally, 30.9%, 30.9%, and 41.2% of participants had at least one risk allele for the coding SNVs rs1805165 (G), rs867529 (G), and rs13045 (A), respectively. Homozygosity for all three coding SNVs was associated with significantly worse GDS (p < 0.001) and more NCI (p < 0.001). By multivariable analysis, the rs13045 A risk allele, current ART use, and Beck Depression Inventory-II value > 13 were independently associated with GDS and NCI (p < 0.001) whereas the other two coding SNVs did not significantly correlate with GDS or NCI after including rs13045 in the model. The coding EIF2AK3 SNVs were associated with worse performance in executive functioning, motor functioning, learning, and verbal fluency. Coding and non-coding SNVs of

Published

2024

2. Tanapox Virus and Yaba Monkey Tumor Virus K3 Orthologs Inhibit Primate Protein Kinase R in a Species-Specific Fashion

Author

Megawati, Dewi, Megawati, Dewi, Stroup, Jeannine N, Park, Chorong, Clarkson, Taylor, Tazi, Loubna, Brennan, Greg, Rothenburg, Stefan, Megawati, Dewi, Megawati, Dewi, Stroup, Jeannine N, Park, Chorong, Clarkson, Taylor, Tazi, Loubna, Brennan, Greg, and Rothenburg, Stefan

Abstract

Yaba monkey tumor virus (YMTV) and Tanapox virus (TPV) are members of the Yatapoxvirus genus and can infect humans and other primates. Despite the threat posed by yatapoxviruses, the factors determining their host range are poorly understood. In this study, we analyzed the ability of YMTV and TPV orthologs of vaccinia virus K3 (called 012 in YMTV and TPV), which share 75% amino acid identity with one another, to inhibit PKR from 15 different primate species. We first used a luciferase-based reporter, and found that YMTV and TPV K3 orthologs inhibited PKR in a species-specific manner and showed distinct PKR inhibition profiles. TPV 012 inhibited PKR from 11 primates, including humans, substantially better than YMTV 012. In contrast, both K3 orthologs inhibited the other four primate PKRs comparably well. Using YMTV 012 and TPV 012 hybrids, we mapped the region responsible for the differential PKR inhibition to the C- terminus of the K3 orthologs. Next, we generated chimeric vaccinia virus strains to investigate whether TPV K3 and YMTV K3 orthologs could rescue the replication of a vaccinia virus strain that lacks PKR inhibitors K3L and E3L. Virus replication in primate-derived cells generally correlated with the patterns observed in the luciferase-based assay. Together, these observations demonstrate that yatapoxvirus K3 orthologs have distinct PKR inhibition profiles and inhibit PKR in a species-specific manner, which may contribute to the differential susceptibility of primate species to yatapoxvirus infections.

Published

2024

3. Regulation of an eukaryotic initiation factor-2 (eIF-2) associated 67 kDa glycoprotein p(67) and its requirement in protein synthesis

Author

Gupta, Swati and Gupta, Swati

Abstract

Eukaryotic initiation factor-2 (eIF-2) associated 67kDa polypeptide (p$\sp{67})$ plays a critical role in the regulation of protein synthesis initiation in mammalian cells. Under certain physiological conditions, phosphorylation of the $\alpha$-subunit of eIF-2 by kinases leads to eIF-2 inactivation and thereby protein synthesis inhibition. p$\sp{67}$ can protect the eIF-2 $\alpha$-subunit from inhibitory phosphorylation and therefore promotes the protein synthesis even in the presence of active eIF-2 kinases. p$\sp{67}$ level in the cells is regulated by two different mechanisms, (i) by activation of a p$\sp{67}$-deglycosylase. Heme-deficient reticulocyte and vaccinia viral infected animal cells use these mechanisms. (ii) at the mRNA level. This mechanism is used during serum starvation and mitogen stimulation of the cells. Direct demonstration and the requirement of p$\sp{67}$ in protein synthesis in vivo was done using cloned p$\sp{67}$ cDNA. The sense and antisense p$\sp{67}$ cDNA were expressed in rat-hepatoma (KRC-7) cells. These phenotypes were then used to investigate the function of p$\sp{67}$ gene in protein synthesis regulation. Expression of the antisense p$\sp{67}$ cDNA in the presence of zinc in PMA-induced serum starved cells completely inhibited induced appearance of p$\sp{67}$ mRNA, p$\sp{67}$ protein and subsequent protein synthesis. Also on expression of sense p$\sp{67}$ cDNA the appearance of p$\sp{67}$ mRNA in the serum starved cells was accompanied by the appearance of p$\sp{67}$ protein and hence the restoration of the rates of total protein synthesis. Thus the loss of p$\sp{67}$ mRNA in serum starved cells is due to loss of p$\sp{67}$ transcription and the p$\sp{67}$ transcription regulates total rate of protein synthesis. The eIF-2 kinase activity was the same in the cells grown in complete medium, after serum starvation and subsequent mitogen stimulation. It is not the level of eIF-2 kinase but the level of p$\sp{67}$ which changes the prot

Published

1997

4. Roles of an eukaryotic initiation factor 2 (eIF-2) associated 67 kDa protein (p(67)) in the regulation of protein synthesis initiation in animal cells

Author

Chakraborty, Arup and Chakraborty, Arup

Abstract

Protein synthesis rapidly shuts off in hemin deficient reticulocyte lysate. It is widely believed that reticulocyte lysate contains a protein synthesis inhibitor in latent form. Under hemin deficiency it becomes activated and phosphorylates the $\alpha$-subunit of eukaryotic initiation factor 2 (eIF-2), thus shutting off protein synthesis. This inhibition can be reversed by the addition of exogenous hemin. Contrary to previous reports, our laboratory has established that this inhibitor, HRI (heme regulated inhibitor), is always active in hemin deficient reticulocyte lysate. But, active HRI can not phosphorylate the eIF-2 $\alpha$-subunit since an eIF-2 associated 67 kDa glycoprotein (p$\sp{67}$) is also present in reticulocyte lysate. This p$\sp{67}$ protects eIF-2 $\alpha$-subunit from kinase catalyzed phosphorylation and thus promotes the protein synthesis in the presence of active eIF-2 kinases such as HRI and dsI (double stranded RNA activated Inhibitor). p$\sp{67}$ is a glycoprotein and contains multiple O-linked GlcNAc moieties. p$\sp{67}$ binds specifically to the eIF-2 $\gamma$-subunit then uses the glycosyl residues to protect the eIF-2 $\alpha$-subunit phosphorylation site from inhibitory phosphorylation by eIF-2 kinases. In hemin deficient reticulocyte lysate, p$\sp{67}$ is rapidly deglycosylated and deglycosylated p$\sp{67}$ can not protect eIF-2 $\alpha$-subunit from eIF-2 kinase catalyzed phosphorylation. The level of control in reticulocyte lysate is at the level of a p$\sp{67}$ deglycosylase present in latent form and activated during hemin deficiency. Another eIF-2 kinase, dsI (double stranded RNA activated inhibitor), plays an important role in protein synthesis regulation during different physiological conditions such as viral infection. eIF-2$\cdot$p$\sp{67}$ complex is resistant to dsI phosphorylation since dsI can not bind to this complex. Autophosphorylated dsI binds to three subunit eIF-2 and then transfers its phosphoryl residue(s) to eIF-2

Published

1994

5. Roles of 67 kDa polypeptide in the regulation of protein synthesis in animal cells and possible mechanism of its activity

Author

Ray, Manas K and Ray, Manas K

Abstract

Addition of partially purified exogenous eIF-2 or the cell supernatant factor (RF), enriched in GEF activity reverses protein synthesis inhibition in heme deficient reticulocyte lysate. This partially purified eIF-2 contains regular three subunits ($\alpha$, $\beta$ and $\gamma$) together with a 67 kDa polypeptide. This 67 kDa polypeptide protects eIF-2 $\alpha$-subunit from eIF-2 kinase catalyzed phosphorylation. This p$\sp{67}$ is a glycoprotein, contains multiple GlcNAc residues. In heme deficient reticulocyte lysate p$\sp{67}$ is deglycosylated and becomes inactive to protect eIF-2 $\alpha$-subunit from phosphorylation. HRI is active in both heme-supplemented and heme-deficient reticulocyte lysate. It is the p$\sp{67}$ which becomes inactive due to deglycosylation in heme-deficient reticulocyte lysate. In heme supplemented reticulocyte lysate p$\sp{67}$ is stable and active to protect $\alpha$-subunit. p$\sp{67}$ is degradable and inducible protein. In quiescent tumor hepatoma cells (KRC-7) p$\sp{67}$ is completely disappeared and becomes prominent in an hour after addition of TPA (phorbol ester). The levels of other polypeptides and interestingly the level of dSI remains essentially same. The level of p$\sp{67}$ correlates directly with the protein synthesis of the cells. At the confluent stage, the protein synthesis rate is maximum, the phosphorylation of eIF-2 $\alpha$-subunit is very low and the p$\sp{67}$ level is very high. At the quiescent stage the protein synthesis rate is very low, phosphorylation of eIF-2 $\alpha$-subunit is maximum and p$\sp{67}$ is almost nonexistent. So the availability of p$\sp{67}$ directly controls the rate of protein synthesis in animal cells. p$\sp{67}$ has to react with eIF-2 for its activity. p$\sp{67}$ reacts with eIF-2 through $\gamma$-subunit. This interaction is protein-protein in nature. The interaction of p$\sp{67}$ with eIF-2 is essential for its activity to protect eIF-2 $\alpha$-subunit from eIF-2 kinase catalyzed p

Published

1991

6. APOBEC3B drives PKR-mediated translation shutdown and protects stress granules in response to viral infection.

Author

Manjunath, Lavanya, Manjunath, Lavanya, Oh, Sunwoo, Ortega, Pedro, Bouin, Alexis, Bournique, Elodie, Sanchez, Ambrocio, Martensen, Pia Møller, Auerbach, Ashley A, Becker, Jordan T, Seldin, Marcus, Harris, Reuben S, Semler, Bert L, Buisson, Rémi, Manjunath, Lavanya, Manjunath, Lavanya, Oh, Sunwoo, Ortega, Pedro, Bouin, Alexis, Bournique, Elodie, Sanchez, Ambrocio, Martensen, Pia Møller, Auerbach, Ashley A, Becker, Jordan T, Seldin, Marcus, Harris, Reuben S, Semler, Bert L, and Buisson, Rémi

Abstract

Double-stranded RNA produced during viral replication and transcription activates both protein kinase R (PKR) and ribonuclease L (RNase L), which limits viral gene expression and replication through host shutoff of translation. In this study, we find that APOBEC3B forms a complex with PABPC1 to stimulate PKR and counterbalances the PKR-suppressing activity of ADAR1 in response to infection by many types of viruses. This leads to translational blockage and the formation of stress granules. Furthermore, we show that APOBEC3B localizes to stress granules through the interaction with PABPC1. APOBEC3B facilitates the formation of protein-RNA condensates with stress granule assembly factor (G3BP1) by protecting mRNA associated with stress granules from RNAse L-induced RNA cleavage during viral infection. These results not only reveal that APOBEC3B is a key regulator of different steps of the innate immune response throughout viral infection but also highlight an alternative mechanism by which APOBEC3B can impact virus replication without editing viral genomes.

Published

2023

7. Targeting the EIF2AK1 Signaling Pathway Rescues Red Blood Cell Production in SF3B1-Mutant Myelodysplastic Syndromes With Ringed Sideroblasts.

Author

Adema, Vera, Adema, Vera, Ma, Feiyang, Kanagal-Shamanna, Rashmi, Thongon, Natthakan, Montalban-Bravo, Guillermo, Yang, Hui, Peslak, Scott A, Wang, Feng, Acha, Pamela, Sole, Francesc, Lockyer, Pamela, Cassari, Margherita, Maciejewski, Jaroslaw P, Visconte, Valeria, Gañán-Gómez, Irene, Song, Yuanbin, Bueso-Ramos, Carlos, Pellegrini, Matteo, Tan, Tuyet M, Bejar, Rafael, Carew, Jennifer S, Halene, Stephanie, Santini, Valeria, Al-Atrash, Gheath, Clise-Dwyer, Karen, Garcia-Manero, Guillermo, Blobel, Gerd A, Colla, Simona, Adema, Vera, Adema, Vera, Ma, Feiyang, Kanagal-Shamanna, Rashmi, Thongon, Natthakan, Montalban-Bravo, Guillermo, Yang, Hui, Peslak, Scott A, Wang, Feng, Acha, Pamela, Sole, Francesc, Lockyer, Pamela, Cassari, Margherita, Maciejewski, Jaroslaw P, Visconte, Valeria, Gañán-Gómez, Irene, Song, Yuanbin, Bueso-Ramos, Carlos, Pellegrini, Matteo, Tan, Tuyet M, Bejar, Rafael, Carew, Jennifer S, Halene, Stephanie, Santini, Valeria, Al-Atrash, Gheath, Clise-Dwyer, Karen, Garcia-Manero, Guillermo, Blobel, Gerd A, and Colla, Simona

Abstract

SF3B1 mutations, which occur in 20% of patients with myelodysplastic syndromes (MDS), are the hallmarks of a specific MDS subtype, MDS with ringed sideroblasts (MDS-RS), which is characterized by the accumulation of erythroid precursors in the bone marrow and primarily affects the elderly population. Here, using single-cell technologies and functional validation studies of primary SF3B1-mutant MDS-RS samples, we show that SF3B1 mutations lead to the activation of the EIF2AK1 pathway in response to heme deficiency and that targeting this pathway rescues aberrant erythroid differentiation and enables the red blood cell maturation of MDS-RS erythroblasts. These data support the development of EIF2AK1 inhibitors to overcome transfusion dependency in patients with SF3B1-mutant MDS-RS with impaired red blood cell production.SignificanceMDS-RS are characterized by significant anemia. Patients with MDS-RS die from a shortage of red blood cells and the side effects of iron overload due to their constant need for transfusions. Our study has implications for the development of therapies to achieve long-lasting hematologic responses. This article is highlighted in the In This Issue feature, p. 476.

Published

2022

8. Roles of an eukaryotic initiation factor 2-associated glycoprotein (p67) in regulation of protein synthesis in vaccinia virus infected animal cells

Author

Bose, Avirup and Bose, Avirup

Abstract

An eukaryotic initiation factor 2 (eIF-2) associated 67 kDa glycoprotein (p67) plays a key role in protein synthesis initiation. In the present work I have studied the role of p67 in regulation of protein synthesis in vaccinia virus infected animal cells. Four different cell lines, KRC-7 (rat hepatoma), L929 (mouse fibroblast), and CV-1 (african green monkey kidney) cell lines were used for this study. These cell lines varied contained widely varying amounts of p67. KRC-7 cells have the highest concentration of endogenous p67 and these cells were resistant to vaccinia virus infection when a low viral titer (5 pfu/cell) was used to infect these cells. The L929 and CV-1 cells were infected under these conditions. KRC-7 cells could be infected only with a higher viral titer (25 pfu/cell) or when the endogenous p67 level was reduced either by serum starving these cells or by expression of p67-antisense DNA. Productive viral infection in all cases studied resulted in the activation of a latent p67-deglycosylase in the infected cells. Once activated, this p67-deglycosylase degiycosylated and consequently inactivated p67. This allowed active eIF-2 kinase(s) in these cells to phosphorylate eIF-2 leading to host protein synthesis shut-off. The virus then used the host machinery to synthesize its own proteins. The activation of p67-deglycosylase was observed within 30 mins of infection and probably preceding viral gene transcription. This indicated that p67-deglycosylase was host gene coded. The mechanism by which high p67 level in the KRC-7 cells prevents productive viral infection at a low viral titer is not clear. Several possibilities have been discussed in Chapter III. Viral DNA was detected in viral resistant KRC-7 cells. However, no viral mRNAs could be detected, indicating that the block in viral replication was at the level of viral gene transcription.

Published

1997

9. A study of the interaction of a 67kDa glycoprotein (p67) with eukaryotic initiation factor 2 (eIF-2) and other cellular proteins

Author

Chattopadhyay, Ansuman and Chattopadhyay, Ansuman

Abstract

The eukaryotic initiation factor 2 (eIF-2) is a hetero-trimer, $\alpha\beta\gamma.$ The eIF-2 kinases (HRI and PKR) phosphorylate specifically the $\alpha$ subunit of eIF-2. This inactivates eIF-2 activity and inhibits protein synthesis. A 67 kDa glycoprotein (p$\sp{67})$ protects eIF-2 $\alpha$ subunit from inhibitory phosphorylation and thus promotes protein synthesis in the presence of active eIF-2 kinase(s). We have now studied the interactions between the eIF-2 subunits and p67 using the yeast two-hybrid system. We expressed the cDNAs for each subunits of eIF-2 and p$\sp{67}$ in yeast as a fusion with the DNA binding or the transcription activation domain of the yeast GAL4 transcription activator. We report that (i) eIF-2 $\gamma$ interacted with all three polypeptides eIF-2 $\alpha,\ \beta$ and p$\sp{67},$ (ii) No interaction was observed between eIF-2 $\alpha,$ eIF-2 $\beta$ and p$\sp{67},$ (iii) Only p$\sp{67}$ formed an oligomer. eIF-2 $\alpha,$ eIF-2 $\beta$ and eIF-2 $\gamma$ did not form oligomers. Molecular weight determination using Sephacryl S-300 gel filtration chromatography revealed that p$\sp{67}$ exits as a dimer. The two hybrid system was also used to screen for binding proteins of the eIF-2 associated 67 kDa glycoprotein, p$\sp{67}$. The plasmid pGBT9-p$\sp{67}$, having a full length rat p$\sp{67}$ fused to the DNA binding domain of GAL4 transcription factor, was prepared. The two hybrid mouse liver cDNA library containing cDNAs fused to the GAL4 trans-activation domain was used. Yeast cells (HF7c) were transformed with the plasmids and screened for clones, whose translational products interact with p$\sp{67}.$ Positive clones were obtained and their DNA sequences were partially determined. Two clones (clone 1 and 4) showed strong sequence identity with rat p$\sp{67}.$ Sequence analysis revealed that the clone 1 shares 98% sequence identity with the amino acid sequence 39-110 of rat p$\sp{67}$ and the clone 4 shares 97% sequence identity with t

Published

1996

10. Activation of IRE1, PERK and salt-inducible kinases leads to Sec body formation in Drosophila S2 cells

Author

Zhang, Chujun, van Leeuwen, Wessel, Blotenburg, Marloes, Aguilera-Gomez, Angelica, Brussee, Sem, Grond, Rianne, Kampinga, Harm H, Rabouille, Catherine, Zhang, Chujun, van Leeuwen, Wessel, Blotenburg, Marloes, Aguilera-Gomez, Angelica, Brussee, Sem, Grond, Rianne, Kampinga, Harm H, and Rabouille, Catherine

Abstract

The phase separation of the non-membrane bound Sec bodies occurs in Drosophila S2 cells by coalescence of components of the endoplasmic reticulum (ER) exit sites under the stress of amino acid starvation. Here, we address which signaling pathways cause Sec body formation and find that two pathways are critical. The first is the activation of the salt-inducible kinases (SIKs; SIK2 and SIK3) by Na+ stress, which, when it is strong, is sufficient. The second is activation of IRE1 and PERK (also known as PEK in flies) downstream of ER stress induced by the absence of amino acids, which needs to be combined with moderate salt stress to induce Sec body formation. SIK, and IRE1 and PERK activation appear to potentiate each other through the stimulation of the unfolded protein response, a key parameter in Sec body formation. This work shows the role of SIKs in phase transition and re-enforces the role of IRE1 and PERK as a metabolic sensor for the level of circulating amino acids and salt. This article has an associated First Person interview with the first author of the paper.

Published

2021

11. Exocyst protein subnetworks integrate Hippo and mTOR signaling to promote virus detection and cancer.

Author

Zaman, Aubhishek, Zaman, Aubhishek, Wu, Xiaofeng, Lemoff, Andrew, Yadavalli, Sivaramakrishna, Lee, Jeon, Wang, Chensu, Cooper, Jonathan, McMillan, Elizabeth A, Yeaman, Charles, Mirzaei, Hamid, White, Michael A, Bivona, Trever G, Zaman, Aubhishek, Zaman, Aubhishek, Wu, Xiaofeng, Lemoff, Andrew, Yadavalli, Sivaramakrishna, Lee, Jeon, Wang, Chensu, Cooper, Jonathan, McMillan, Elizabeth A, Yeaman, Charles, Mirzaei, Hamid, White, Michael A, and Bivona, Trever G

Abstract

The exocyst is an evolutionarily conserved protein complex that regulates vesicular trafficking and scaffolds signal transduction. Key upstream components of the exocyst include monomeric RAL GTPases, which help mount cell-autonomous responses to trophic and immunogenic signals. Here, we present a quantitative proteomics-based characterization of dynamic and signal-dependent exocyst protein interactomes. Under viral infection, an Exo84 exocyst subcomplex assembles the immune kinase Protein Kinase R (PKR) together with the Hippo kinase Macrophage Stimulating 1 (MST1). PKR phosphorylates MST1 to activate Hippo signaling and inactivate Yes Associated Protein 1 (YAP1). By contrast, a Sec5 exocyst subcomplex recruits another immune kinase, TANK binding kinase 1 (TBK1), which interacted with and activated mammalian target of rapamycin (mTOR). RALB was necessary and sufficient for induction of Hippo and mTOR signaling through parallel exocyst subcomplex engagement, supporting the cellular response to virus infection and oncogenic signaling. This study highlights RALB-exocyst signaling subcomplexes as mechanisms for the integrated engagement of Hippo and mTOR signaling in cells challenged by viral pathogens or oncogenic signaling.

Published

2021

12. Activation of IRE1, PERK and salt-inducible kinases leads to Sec body formation in Drosophila S2 cells

Author

Zhang, Chujun, van Leeuwen, Wessel, Blotenburg, Marloes, Aguilera-Gomez, Angelica, Brussee, Sem, Grond, Rianne, Kampinga, Harm H, Rabouille, Catherine, Zhang, Chujun, van Leeuwen, Wessel, Blotenburg, Marloes, Aguilera-Gomez, Angelica, Brussee, Sem, Grond, Rianne, Kampinga, Harm H, and Rabouille, Catherine

Abstract

The phase separation of the non-membrane bound Sec bodies occurs in Drosophila S2 cells by coalescence of components of the endoplasmic reticulum (ER) exit sites under the stress of amino acid starvation. Here, we address which signaling pathways cause Sec body formation and find that two pathways are critical. The first is the activation of the salt-inducible kinases (SIKs; SIK2 and SIK3) by Na+ stress, which, when it is strong, is sufficient. The second is activation of IRE1 and PERK (also known as PEK in flies) downstream of ER stress induced by the absence of amino acids, which needs to be combined with moderate salt stress to induce Sec body formation. SIK, and IRE1 and PERK activation appear to potentiate each other through the stimulation of the unfolded protein response, a key parameter in Sec body formation. This work shows the role of SIKs in phase transition and re-enforces the role of IRE1 and PERK as a metabolic sensor for the level of circulating amino acids and salt. This article has an associated First Person interview with the first author of the paper.

Published

2021

13. PERK-mediated induction of microRNA-483 disrupts cellular ATP homeostasis during the unfolded protein response.

Author

Hiramatsu, Nobuhiko, Hiramatsu, Nobuhiko, Chiang, Karen, Aivati, Cathrine, Rodvold, Jeffrey J, Lee, Ji-Min, Han, Jaeseok, Chea, Leon, Zanetti, Maurizio, Koo, Edward H, Lin, Jonathan H, Hiramatsu, Nobuhiko, Hiramatsu, Nobuhiko, Chiang, Karen, Aivati, Cathrine, Rodvold, Jeffrey J, Lee, Ji-Min, Han, Jaeseok, Chea, Leon, Zanetti, Maurizio, Koo, Edward H, and Lin, Jonathan H

Abstract

Endoplasmic reticulum (ER) stress activates the unfolded protein response (UPR), which reduces levels of misfolded proteins. However, if ER homeostasis is not restored and the UPR remains chronically activated, cells undergo apoptosis. The UPR regulator, PKR-like endoplasmic reticulum kinase (PERK), plays an important role in promoting cell death when persistently activated; however, the underlying mechanisms are poorly understood. Here, we profiled the microRNA (miRNA) transcriptome in human cells exposed to ER stress and identified miRNAs that are selectively induced by PERK signaling. We found that expression of a PERK-induced miRNA, miR-483, promotes apoptosis in human cells. miR-483 induction was mediated by a transcription factor downstream of PERK, activating transcription factor 4 (ATF4), but not by the CHOP transcription factor. We identified the creatine kinase brain-type (CKB) gene, encoding an enzyme that maintains cellular ATP reserves through phosphocreatine production, as being repressed during the UPR and targeted by miR-483. We found that ER stress, selective PERK activation, and CKB knockdown all decrease cellular ATP levels, leading to increased vulnerability to ER stress-induced cell death. Our findings identify miR-483 as a downstream target of the PERK branch of the UPR. We propose that disruption of cellular ATP homeostasis through miR-483-mediated CKB silencing promotes ER stress-induced apoptosis.

Published

2020

14. Rapid, Seamless Generation of Recombinant Poxviruses using Host Range and Visual Selection.

Author

Vipat, Sameera, Vipat, Sameera, Brennan, Greg, Park, Chorong, Haller, Sherry L, Rothenburg, Stefan, Vipat, Sameera, Vipat, Sameera, Brennan, Greg, Park, Chorong, Haller, Sherry L, and Rothenburg, Stefan

Abstract

Vaccinia virus (VACV) was instrumental in eradicating variola virus (VARV), the causative agent of smallpox, from nature. Since its first use as a vaccine, VACV has been developed as a vector for therapeutic vaccines and as an oncolytic virus. These applications take advantage of VACV's easily manipulated genome and broad host range as an outstanding platform to generate recombinant viruses with a variety of therapeutic applications. Several methods have been developed to generate recombinant VACV, including marker selection methods and transient dominant selection. Here, we present a refinement of a host range selection method coupled with visual identification of recombinant viruses. Our method takes advantage of selective pressure generated by the host antiviral protein kinase R (PKR) coupled with a fluorescent fusion gene expressing mCherry-tagged E3L, one of two VACV PKR antagonists. The cassette, including the gene of interest and the mCherry-E3L fusion is flanked by sequences derived from the VACV genome. Between the gene of interest and mCherry-E3L is a smaller region that is identical to the first ~150 nucleotides of the 3' arm, to promote homologous recombination and loss of the mCherry-E3L gene after selection. We demonstrate that this method permits efficient, seamless generation of rVACV in a variety of cell types without requiring drug selection or extensive screening for mutant viruses.

Published

2020

15. Activation of the ISR mediates the behavioral and neurophysiological abnormalities in Down syndrome.

Author

Zhu, Ping Jun, Zhu, Ping Jun, Khatiwada, Sanjeev, Cui, Ya, Reineke, Lucas C, Dooling, Sean W, Kim, Jean J, Li, Wei, Walter, Peter, Costa-Mattioli, Mauro, Zhu, Ping Jun, Zhu, Ping Jun, Khatiwada, Sanjeev, Cui, Ya, Reineke, Lucas C, Dooling, Sean W, Kim, Jean J, Li, Wei, Walter, Peter, and Costa-Mattioli, Mauro

Abstract

Down syndrome (DS) is the most common genetic cause of intellectual disability. Protein homeostasis is essential for normal brain function, but little is known about its role in DS pathophysiology. In this study, we found that the integrated stress response (ISR)-a signaling network that maintains proteostasis-was activated in the brains of DS mice and individuals with DS, reprogramming translation. Genetic and pharmacological suppression of the ISR, by inhibiting the ISR-inducing double-stranded RNA-activated protein kinase or boosting the function of the eukaryotic translation initiation factor eIF2-eIF2B complex, reversed the changes in translation and inhibitory synaptic transmission and rescued the synaptic plasticity and long-term memory deficits in DS mice. Thus, the ISR plays a crucial role in DS, which suggests that tuning of the ISR may provide a promising therapeutic intervention.

Published

2019

16. Tauopathy-associated PERK alleles are functional hypomorphs that increase neuronal vulnerability to ER stress.

Author

Yuan, Shauna H, Yuan, Shauna H, Hiramatsu, Nobuhiko, Liu, Qing, Sun, Xuehan Victoria, Lenh, David, Chan, Priscilla, Chiang, Karen, Koo, Edward H, Kao, Aimee W, Litvan, Irene, Lin, Jonathan H, Yuan, Shauna H, Yuan, Shauna H, Hiramatsu, Nobuhiko, Liu, Qing, Sun, Xuehan Victoria, Lenh, David, Chan, Priscilla, Chiang, Karen, Koo, Edward H, Kao, Aimee W, Litvan, Irene, and Lin, Jonathan H

Abstract

Tauopathies are neurodegenerative diseases characterized by tau protein pathology in the nervous system. EIF2AK3 (eukaryotic translation initiation factor 2 alpha kinase 3), also known as PERK (protein kinase R-like endoplasmic reticulum kinase), was identified by genome-wide association study as a genetic risk factor in several tauopathies. PERK is a key regulator of the Unfolded Protein Response (UPR), an intracellular signal transduction mechanism that protects cells from endoplasmic reticulum (ER) stress. PERK variants had previously been identified in Wolcott-Rallison Syndrome, a rare autosomal recessive metabolic disorder, and these variants completely abrogated the function of PERK's kinase domain or prevented PERK expression. In contrast, the PERK tauopathy risk variants were distinct from the Wolcott-Rallison variants and introduced missense alterations throughout the PERK protein. The function of PERK tauopathy variants and their effects on neurodegeneration are unknown. Here, we discovered that tauopathy-associated PERK alleles showed reduced signaling activity and increased PERK protein turnover compared to protective PERK alleles. We found that iPSC-derived neurons carrying PERK risk alleles were highly vulnerable to ER stress-induced injury with increased tau pathology. We found that chemical inhibition of PERK in human iPSC-derived neurons also increased neuronal cell death in response to ER stress. Our results indicate that tauopathy-associated PERK alleles are functional hypomorphs during the UPR. We propose that reduced PERK function leads to neurodegeneration by increasing neuronal vulnerability to ER stress-associated damage. In this view, therapies to enhance PERK signaling would benefit at-risk carriers of hypomorphic alleles.

Published

2018

17. Complement activation during ischemia/reperfusion injury induces pericyte-to-myofibroblast transdifferentiation regulating peritubular capillary Lumen Reduction Through pERK Signaling

Author

Castellano, G., Franzin, R., Stasi, A., Divella, C., Sallustio, F., Pontrelli, P., Lucarelli, G., Battaglia, M., Staffieri, F., Crovace, A., Stallone, G., Seelen, M., Daha, M. R., Grandaliano, G. (ORCID:0000-0003-1213-2177), Gesualdo, L., Castellano, G., Franzin, R., Stasi, A., Divella, C., Sallustio, F., Pontrelli, P., Lucarelli, G., Battaglia, M., Staffieri, F., Crovace, A., Stallone, G., Seelen, M., Daha, M. R., Grandaliano, G. (ORCID:0000-0003-1213-2177), and Gesualdo, L.

Abstract

Pericytes are one of the principal sources of scar-forming myofibroblasts in chronic kidneys disease. However, the modulation of pericyte-to-myofibroblast transdifferentiation (PMT) in the early phases of acute kidney injury is poorly understood. Here, we investigated the role of complement in inducing PMT after transplantation. Using a swine model of renal ischemia/reperfusion (I/R) injury, we found the occurrence of PMT after 24 h of I/R injury as demonstrated by reduction of PDGFRβ+/NG2+ cells with increase in myofibroblasts marker aSMA. In addition, PMT was associated with significant reduction in peritubular capillary luminal diameter. Treatment by C1-inhibitor (C1-INH) significantly preserved the phenotype of pericytes maintaining microvascular density and capillary lumen area at tubulointerstitial level. In vitro, C5a transdifferentiated human pericytes in myofibroblasts, with increased aSMA expression in stress fibers, collagen I production, and decreased antifibrotic protein Id2. The C5a-induced PMT was driven by extracellular signal-regulated kinases phosphorylation leading to increase in collagen I release that required both non-canonical and canonical TGFβ pathways. These results showed that pericytes are a pivotal target of complement activation leading to a profibrotic maladaptive cellular response. Our studies suggest that C1-INH may be a potential therapeutic strategy to counteract the development of PMT and capillary lumen reduction in I/R injury.

Published

2018

18. Tauopathy-associated PERK alleles are functional hypomorphs that increase neuronal vulnerability to ER stress.

Author

Yuan, Shauna H, Yuan, Shauna H, Hiramatsu, Nobuhiko, Liu, Qing, Sun, Xuehan Victoria, Lenh, David, Chan, Priscilla, Chiang, Karen, Koo, Edward H, Kao, Aimee W, Litvan, Irene, Lin, Jonathan H, Yuan, Shauna H, Yuan, Shauna H, Hiramatsu, Nobuhiko, Liu, Qing, Sun, Xuehan Victoria, Lenh, David, Chan, Priscilla, Chiang, Karen, Koo, Edward H, Kao, Aimee W, Litvan, Irene, and Lin, Jonathan H

Abstract

Tauopathies are neurodegenerative diseases characterized by tau protein pathology in the nervous system. EIF2AK3 (eukaryotic translation initiation factor 2 alpha kinase 3), also known as PERK (protein kinase R-like endoplasmic reticulum kinase), was identified by genome-wide association study as a genetic risk factor in several tauopathies. PERK is a key regulator of the Unfolded Protein Response (UPR), an intracellular signal transduction mechanism that protects cells from endoplasmic reticulum (ER) stress. PERK variants had previously been identified in Wolcott-Rallison Syndrome, a rare autosomal recessive metabolic disorder, and these variants completely abrogated the function of PERK's kinase domain or prevented PERK expression. In contrast, the PERK tauopathy risk variants were distinct from the Wolcott-Rallison variants and introduced missense alterations throughout the PERK protein. The function of PERK tauopathy variants and their effects on neurodegeneration are unknown. Here, we discovered that tauopathy-associated PERK alleles showed reduced signaling activity and increased PERK protein turnover compared to protective PERK alleles. We found that iPSC-derived neurons carrying PERK risk alleles were highly vulnerable to ER stress-induced injury with increased tau pathology. We found that chemical inhibition of PERK in human iPSC-derived neurons also increased neuronal cell death in response to ER stress. Our results indicate that tauopathy-associated PERK alleles are functional hypomorphs during the UPR. We propose that reduced PERK function leads to neurodegeneration by increasing neuronal vulnerability to ER stress-associated damage. In this view, therapies to enhance PERK signaling would benefit at-risk carriers of hypomorphic alleles.

Published

2018

19. Protein kinase R-like endoplasmic reticulum kinase is a mediator of stretch in ventilator-induced lung injury

Author

Dolinay, Tamás, Dolinay, Tamás, Aonbangkhen, Chanat, Zacharias, William, Cantu, Edward, Pogoriler, Jennifer, Stablow, Alec, Lawrence, Gladys G, Suzuki, Yoshikazu, Chenoweth, David M, Morrisey, Edward, Christie, Jason D, Beers, Michael F, Margulies, Susan S, Dolinay, Tamás, Dolinay, Tamás, Aonbangkhen, Chanat, Zacharias, William, Cantu, Edward, Pogoriler, Jennifer, Stablow, Alec, Lawrence, Gladys G, Suzuki, Yoshikazu, Chenoweth, David M, Morrisey, Edward, Christie, Jason D, Beers, Michael F, and Margulies, Susan S

Abstract

BackgroundAcute respiratory distress syndrome (ARDS) is a severe form of lung injury characterized by damage to the epithelial barrier with subsequent pulmonary edema and hypoxic respiratory failure. ARDS is a significant medical problem in intensive care units with associated high care costs. There are many potential causes of ARDS; however, alveolar injury associated with mechanical ventilation, termed ventilator-induced lung injury (VILI), remains a well-recognized contributor. It is thus critical to understand the mechanism of VILI. Based on our published preliminary data, we hypothesized that the endoplasmic reticulum (ER) stress response molecule Protein Kinase R-like Endoplasmic Reticulum Kinase (PERK) plays a role in transmitting mechanosensory signals the alveolar epithelium.MethodsER stress signal responses to mechanical stretch were studied in ex-vivo ventilated pig lungs. To explore the effect of PERK inhibition on VILI, we ventilated live rats and compared lung injury parameters to non-ventilated controls. The effect of stretch-induced epithelial ER Ca2+ signaling on PERK was studied in stretched alveolar epithelial monolayers. To confirm the activation of PERK in human disease, ER stress signaling was compared between ARDS and non-ARDS lungs.ResultsOur studies revealed increased PERK-specific ER stress signaling in response to overstretch. PERK inhibition resulted in dose-dependent improvement of alveolar inflammation and permeability. Our data indicate that stretch-induced epithelial ER Ca2+ release is an activator of PERK. Experiments with human lung tissue confirmed PERK activation by ARDS.ConclusionOur study provides evidences that PERK is a mediator stretch signals in the alveolar epithelium.

Published

2018

20. Intercellular transmission of the unfolded protein response promotes survival and drug resistance in cancer cells.

Author

Rodvold, Jeffrey J, Rodvold, Jeffrey J, Chiu, Kevin T, Hiramatsu, Nobuhiko, Nussbacher, Julia K, Galimberti, Valentina, Mahadevan, Navin R, Willert, Karl, Lin, Jonathan H, Zanetti, Maurizio, Rodvold, Jeffrey J, Rodvold, Jeffrey J, Chiu, Kevin T, Hiramatsu, Nobuhiko, Nussbacher, Julia K, Galimberti, Valentina, Mahadevan, Navin R, Willert, Karl, Lin, Jonathan H, and Zanetti, Maurizio

Abstract

Increased protein translation in cells and various factors in the tumor microenvironment can induce endoplasmic reticulum (ER) stress, which initiates the unfolded protein response (UPR). We have previously reported that factors released from cancer cells mounting a UPR induce a de novo UPR in bone marrow-derived myeloid cells, macrophages, and dendritic cells that facilitates protumorigenic characteristics in culture and tumor growth in vivo. We investigated whether this intercellular signaling, which we have termed transmissible ER stress (TERS), also operates between cancer cells and what its functional consequences were within the tumor. We found that TERS signaling induced a UPR in recipient human prostate cancer cells that included the cell surface expression of the chaperone GRP78. TERS also activated Wnt signaling in recipient cancer cells and enhanced resistance to nutrient starvation and common chemotherapies such as the proteasome inhibitor bortezomib and the microtubule inhibitor paclitaxel. TERS-induced activation of Wnt signaling required the UPR kinase and endonuclease IRE1. However, TERS-induced enhancement of cell survival was predominantly mediated by the UPR kinase PERK and a reduction in the abundance of the transcription factor ATF4, which prevented the activation of the transcription factor CHOP and, consequently, the induction of apoptosis. When implanted in mice, TERS-primed cancer cells gave rise to faster growing tumors than did vehicle-primed cancer cells. Collectively, our data demonstrate that TERS is a mechanism of intercellular communication through which tumor cells can adapt to stressful environments.

Published

2017

21. Post-crizotinib management of effective ceritinib therapy in a patient with ALK-positive non-small cell lung cancer.

Author

Won, Brian, Won, Brian, Mambetsariev, Isa, Salgia, Ravi, Won, Brian, Won, Brian, Mambetsariev, Isa, and Salgia, Ravi

Abstract

BackgroundWe report the re-biopsied diagnosis of a patient with anaplastic lymphoma receptor tyrosine kinase (ALK)-positive lung adenocarcinoma successfully treated with ceritinib 450 mg/day taken with food following disease progression and gastrointestinal intolerance to crizotinib.Case presentationA 74-year old female patient initially diagnosed with ALK-negative lung adenocarcinoma responded to initial standard chemotherapy. The patient was subsequently re-tested by next generation sequencing (NGS) and found to have ALK EIF2AK3-ALK fusion, and responded to crizotinib, but ultimately progressed and showed intolerance to this ALK inhibitor. She was then successfully treated with ceritinib 450 mg/day taken with food, has not suffered from any further gastrointestinal side-effects, and remains on ceritinib treatment after 12 months.ConclusionsSecond-line ceritinib treatment, when administered at 450 mg/day with food, is both well tolerated and efficacious in a patient with previously treated lung adenocarcinoma who had discontinued crizotinib due to disease progression and gastrointestinal adverse effects (AEs).

Published

2016

22. Post-crizotinib management of effective ceritinib therapy in a patient with ALK-positive non-small cell lung cancer.

Author

Won, Brian, Won, Brian, Mambetsariev, Isa, Salgia, Ravi, Won, Brian, Won, Brian, Mambetsariev, Isa, and Salgia, Ravi

Abstract

BackgroundWe report the re-biopsied diagnosis of a patient with anaplastic lymphoma receptor tyrosine kinase (ALK)-positive lung adenocarcinoma successfully treated with ceritinib 450 mg/day taken with food following disease progression and gastrointestinal intolerance to crizotinib.Case presentationA 74-year old female patient initially diagnosed with ALK-negative lung adenocarcinoma responded to initial standard chemotherapy. The patient was subsequently re-tested by next generation sequencing (NGS) and found to have ALK EIF2AK3-ALK fusion, and responded to crizotinib, but ultimately progressed and showed intolerance to this ALK inhibitor. She was then successfully treated with ceritinib 450 mg/day taken with food, has not suffered from any further gastrointestinal side-effects, and remains on ceritinib treatment after 12 months.ConclusionsSecond-line ceritinib treatment, when administered at 450 mg/day with food, is both well tolerated and efficacious in a patient with previously treated lung adenocarcinoma who had discontinued crizotinib due to disease progression and gastrointestinal adverse effects (AEs).

Published

2016

23. Myxoma virus M156 is a specific inhibitor of rabbit PKR but contains a loss-of-function mutation in Australian virus isolates.

Author

Peng, Chen, Peng, Chen, Haller, Sherry L, Rahman, Masmudur M, McFadden, Grant, Rothenburg, Stefan, Peng, Chen, Peng, Chen, Haller, Sherry L, Rahman, Masmudur M, McFadden, Grant, and Rothenburg, Stefan

Abstract

Myxoma virus (MYXV) is a rabbit-specific poxvirus, which is highly virulent in European rabbits. The attenuation of MYXV and the increased resistance of rabbits following the release of MYXV in Australia is one of the best-documented examples of host-pathogen coevolution. To elucidate the molecular mechanisms that contribute to the restriction of MYXV infection to rabbits and MYXV attenuation in the field, we have studied the interaction of the MYXV protein M156 with the host antiviral protein kinase R (PKR). In yeast and cell-culture transfection assays, M156 only inhibited rabbit PKR but not PKR from other tested mammalian species. Infection assays with human HeLa PKR knock-down cells, which were stably transfected with human or rabbit PKR, revealed that only human but not rabbit PKR was able to restrict MYXV infection, whereas both PKRs were able to restrict replication of a vaccinia virus (VACV) strain that lacks the PKR inhibitors E3 and K3. Inactivation of M156R led to MYXV virus attenuation in rabbit cells, which was rescued by the ectopic expression of VACV E3 and K3. We further show that a mutation in the M156 encoding gene that was identified in more than 50% of MYXV field isolates from Australia resulted in an M156 variant that lost its ability to inhibit rabbit PKR and led to virus attenuation. The species-specific inhibition of rabbit PKR by M156 and the M156 loss-of-function in Australian MYXV field isolates might thus contribute to the species specificity of MYXV and to the attenuation in the field, respectively.

Published

2016

24. A novel role of c-FLIP protein in regulation of ER stress response

Author

Conti, S., Petrungaro, S., Marini, E. S., Masciarelli, Silvia, Tomaipitinca, L., Filippini, A., Giampietri, C., Ziparo, E., Masciarelli S., Conti, S., Petrungaro, S., Marini, E. S., Masciarelli, Silvia, Tomaipitinca, L., Filippini, A., Giampietri, C., Ziparo, E., and Masciarelli S.

Abstract

Cellular-Flice-like inhibitory protein (c-FLIP) is an apoptosis modulator known to inhibit the extrinsic apoptotic pathway thus blocking Caspase-8 processing in the Death Inducing Signalling Complex (DISC). We previously demonstrated that c-FLIP localizes at the endoplasmic reticulum (ER) and that c-FLIP-deficient mouse embryonic fibroblasts (MEFs) display an enlarged ER morphology. In the present study, we have addressed the consequences of c-FLIP ablation in the ER stress response by investigating the effects of pharmacologically-induced ER stress in Wild Type (WT) and c-FLIP. -/- MEFs. Surprisingly, c-FLIP. -/- MEFs were found to be strikingly more resistant than WT MEFs to ER stress-mediated apoptosis. Analysis of Unfolded Protein Response (UPR) pathways revealed that Pancreatic ER Kinase (PERK) and Inositol-Requiring Enzyme 1 (IRE1) branch signalling is compromised in c-FLIP. -/- cells when compared with WT cells. We found that c-FLIP modulates the PERK pathway by interfering with the activity of the serine threonine kinase AKT. Indeed, c-FLIP. -/- MEFs display higher levels of active AKT than WT MEFs upon ER stress, while treatment with a specific AKT inhibitor of c-FLIP. -/- MEFs subjected to ER stress restores the PERK but not the IRE1 pathway. Importantly, the AKT inhibitor or dominant negative AKT transfection sensitizes c-FLIP. -/- cells to ER stress-induced cell death while the expression of a constitutively active AKT reduces WT cells sensitivity to ER stress-induced death. Thus, our results demonstrate that c-FLIP modulation of AKT activity is crucial in controlling PERK signalling and sensitivity to ER stress, and highlight c-FLIP as a novel molecular player in PERK and IRE1-mediated ER stress response.

Published

2016

25. Multiple Mechanisms of Unfolded Protein Response-Induced Cell Death.

Author

Hiramatsu, Nobuhiko, Hiramatsu, Nobuhiko, Chiang, Wei-Chieh, Kurt, Timothy D, Sigurdson, Christina J, Lin, Jonathan H, Hiramatsu, Nobuhiko, Hiramatsu, Nobuhiko, Chiang, Wei-Chieh, Kurt, Timothy D, Sigurdson, Christina J, and Lin, Jonathan H

Abstract

Eukaryotic cells fold and assemble membrane and secreted proteins in the endoplasmic reticulum (ER), before delivery to other cellular compartments or the extracellular environment. Correctly folded proteins are released from the ER, and poorly folded proteins are retained until they achieve stable conformations; irreparably misfolded proteins are targeted for degradation. Diverse pathological insults, such as amino acid mutations, hypoxia, or infection, can overwhelm ER protein quality control, leading to misfolded protein buildup, causing ER stress. To cope with ER stress, eukaryotic cells activate the unfolded protein response (UPR) by increasing levels of ER protein-folding enzymes and chaperones, enhancing the degradation of misfolded proteins, and reducing protein translation. In mammalian cells, three ER transmembrane proteins, inositol-requiring enzyme-1 (IRE1; official name ERN1), PKR-like ER kinase (PERK; official name EIF2AK3), and activating transcription factor-6, control the UPR. The UPR signaling triggers a set of prodeath programs when the cells fail to successfully adapt to ER stress or restore homeostasis. ER stress and UPR signaling are implicated in the pathogenesis of diverse diseases, including neurodegeneration, cancer, diabetes, and inflammation. This review discusses the current understanding in both adaptive and apoptotic responses as well as the molecular mechanisms instigating apoptosis via IRE1 and PERK signaling. We also examine how IRE1 and PERK signaling may be differentially used during neurodegeneration arising in retinitis pigmentosa and prion infection.

Published

2015

26. Modulation of the unfolded protein response impedes tumor cell adaptation to proteotoxic stress: a PERK for hepatocellular carcinoma therapy.

Author

UCL - SSS/IREC - Institut de recherche expérimentale et clinique, Vandewynckel, Yves-Paul, Laukens, Debby, Bogaerts, Eliene, Paridaens, Annelies, Van den Bussche, Anja, Verhelst, Xavier, Van Steenkiste, Christophe, Descamps, Benedicte, Vanhove, Chris, Libbrecht, Louis, De Rycke, Riet, Lambrecht, Bart N, Geerts, Anja, Janssens, Sophie, Van Vlierberghe, Hans, UCL - SSS/IREC - Institut de recherche expérimentale et clinique, Vandewynckel, Yves-Paul, Laukens, Debby, Bogaerts, Eliene, Paridaens, Annelies, Van den Bussche, Anja, Verhelst, Xavier, Van Steenkiste, Christophe, Descamps, Benedicte, Vanhove, Chris, Libbrecht, Louis, De Rycke, Riet, Lambrecht, Bart N, Geerts, Anja, Janssens, Sophie, and Van Vlierberghe, Hans

Abstract

BACKGROUND: Functional disturbances of the endoplasmic reticulum (ER) lead to activation of the unfolded protein response (UPR), which is involved in the consecutive steps of carcinogenesis. In human hepatocellular carcinoma (HCC), the UPR is shown to be activated; however, little is known about the UPR kinetics and effects of UPR modulation in HCC. METHODS: We sequentially monitored the UPR over time in an orthotopic mouse model for HCC and explored the effects of UPR modulation on cell viability and proliferation in vitro and in the mouse model. RESULTS: The expression of ER-resident chaperones peaked during tumor initiation and increased further during tumor progression, predominantly within the nodules. A peak in Ire1 signaling was observed during tumor initiation. The Perk pathway was activated during tumor progression, and the proapoptotic target Chop was upregulated from week 5 and continued to rise, especially in the tumors. The Atf6 pathway was modestly activated only after tumor initiation. Consistent with the UPR activation, electron microscopy demonstrated ER expansion and reorganization in HCC cells in vivo. Strikingly, under ER stress or hypoxia, the Perk inhibitor and not the Ire1 inhibitor reduced cell viability and proliferation via escalating proteotoxic stress in vitro. Notably, the Perk inhibitor significantly decreased tumor burden in the mouse model. CONCLUSION: We provide the first evaluation of the UPR dynamics in a long-term cancer model and identified a small molecule inhibitor of Perk as a promising strategy for HCC therapy.

Published

2015

27. Multiple Mechanisms of Unfolded Protein Response-Induced Cell Death.

Author

Hiramatsu, Nobuhiko, Hiramatsu, Nobuhiko, Chiang, Wei-Chieh, Kurt, Timothy D, Sigurdson, Christina J, Lin, Jonathan H, Hiramatsu, Nobuhiko, Hiramatsu, Nobuhiko, Chiang, Wei-Chieh, Kurt, Timothy D, Sigurdson, Christina J, and Lin, Jonathan H

Abstract

Eukaryotic cells fold and assemble membrane and secreted proteins in the endoplasmic reticulum (ER), before delivery to other cellular compartments or the extracellular environment. Correctly folded proteins are released from the ER, and poorly folded proteins are retained until they achieve stable conformations; irreparably misfolded proteins are targeted for degradation. Diverse pathological insults, such as amino acid mutations, hypoxia, or infection, can overwhelm ER protein quality control, leading to misfolded protein buildup, causing ER stress. To cope with ER stress, eukaryotic cells activate the unfolded protein response (UPR) by increasing levels of ER protein-folding enzymes and chaperones, enhancing the degradation of misfolded proteins, and reducing protein translation. In mammalian cells, three ER transmembrane proteins, inositol-requiring enzyme-1 (IRE1; official name ERN1), PKR-like ER kinase (PERK; official name EIF2AK3), and activating transcription factor-6, control the UPR. The UPR signaling triggers a set of prodeath programs when the cells fail to successfully adapt to ER stress or restore homeostasis. ER stress and UPR signaling are implicated in the pathogenesis of diverse diseases, including neurodegeneration, cancer, diabetes, and inflammation. This review discusses the current understanding in both adaptive and apoptotic responses as well as the molecular mechanisms instigating apoptosis via IRE1 and PERK signaling. We also examine how IRE1 and PERK signaling may be differentially used during neurodegeneration arising in retinitis pigmentosa and prion infection.

Published

2015

28. Feedback regulation on PTEN/AKT pathway by the ER stress kinase PERK mediated by interaction with the Vault complex

Author

Zhang, Wei, Neo, Suat Peng, Gunaratne, Jayantha, Poulsen, Anders, Boping, Liu, Ong, Esther Hongqian, Sangthongpitag, Kanda, Pendharkar, Vishal, Hill, Jeffrey, Cohen, Stephen Michael, Zhang, Wei, Neo, Suat Peng, Gunaratne, Jayantha, Poulsen, Anders, Boping, Liu, Ong, Esther Hongqian, Sangthongpitag, Kanda, Pendharkar, Vishal, Hill, Jeffrey, and Cohen, Stephen Michael

Abstract

The high proliferation rate of cancer cells, together with environmental factors such as hypoxia and nutrient deprivation can cause Endoplasmic Reticulum (ER) stress. The protein kinase PERK is an essential mediator in one of the three ER stress response pathways. Genetic and pharmacological inhibition of PERK has been reported to limit tumor growth in xenograft models. Here we provide evidence that inactive PERK interacts with the nuclear pore-associated Vault complex protein and that this compromises Vault-mediated nuclear transport of PTEN. Pharmacological inhibition of PERK under ER stress results is abnormal sequestration of the Vault complex, leading to increased cytoplasmic PTEN activity and lower AKT activation. As the PI3K/PTEN/AKT pathway is crucial for many aspects of cell growth and survival, this unexpected effect of PERK inhibitors on AKT activity may have implications for their potential use as therapeutic agents.

Published

2015

29. The effects of IRE1, ATF6, and PERK signaling on adRP-linked rhodopsins.

Author

Jerry Chiang, Wei-Chieh, Jerry Chiang, Wei-Chieh, Lin, Jonathan H, Jerry Chiang, Wei-Chieh, Jerry Chiang, Wei-Chieh, and Lin, Jonathan H

Abstract

Many mutations in rhodopsin gene linked to retinitis pigmentosa (RP) cause rhodopsin misfolding. Rod photoreceptor cells expressing misfolded rhodopsin eventually die. Identifying mechanisms to prevent rhodopsin misfolding or to remove irreparably misfolded rhodopsin could provide new therapeutic strategies. IRE1, ATF6, and PERK signaling pathways, collectively called the unfolded protein response (UPR), regulate the functions of endoplasmic reticulum, responsible for accurate folding of membrane proteins such as rhodopsin. We used chemical and genetic approaches to selectively activate IRE1, ATF6, or PERK signaling pathways one at a time and analyzed their effects on mutant rhodopsin linked to RP. We found that both artificial IRE1 and ATF6 signaling promoted the degradation of mutant rhodopsin with lesser effects on wild-type rhodopsin. Furthermore, IRE1 and ATF6 signaling preferentially reduced levels of aggregated rhodopsins. By contrast, PERK signaling reduced levels of wild-type and mutant rhodopsin. These studies indicate that activation of either IRE1, ATF6, or PERK prevents mutant rhodopsin from accumulating in the cells. In addition, activation of IRE1 or ATF6 can selectively remove aggregated or mutant rhodopsin from the cells and may be useful in treating RP associated with rhodopsin protein misfolding.

Published

2014

30. The effects of IRE1, ATF6, and PERK signaling on adRP-linked rhodopsins.

Author

Jerry Chiang, Wei-Chieh, Jerry Chiang, Wei-Chieh, Lin, Jonathan H, Jerry Chiang, Wei-Chieh, Jerry Chiang, Wei-Chieh, and Lin, Jonathan H

Abstract

Many mutations in rhodopsin gene linked to retinitis pigmentosa (RP) cause rhodopsin misfolding. Rod photoreceptor cells expressing misfolded rhodopsin eventually die. Identifying mechanisms to prevent rhodopsin misfolding or to remove irreparably misfolded rhodopsin could provide new therapeutic strategies. IRE1, ATF6, and PERK signaling pathways, collectively called the unfolded protein response (UPR), regulate the functions of endoplasmic reticulum, responsible for accurate folding of membrane proteins such as rhodopsin. We used chemical and genetic approaches to selectively activate IRE1, ATF6, or PERK signaling pathways one at a time and analyzed their effects on mutant rhodopsin linked to RP. We found that both artificial IRE1 and ATF6 signaling promoted the degradation of mutant rhodopsin with lesser effects on wild-type rhodopsin. Furthermore, IRE1 and ATF6 signaling preferentially reduced levels of aggregated rhodopsins. By contrast, PERK signaling reduced levels of wild-type and mutant rhodopsin. These studies indicate that activation of either IRE1, ATF6, or PERK prevents mutant rhodopsin from accumulating in the cells. In addition, activation of IRE1 or ATF6 can selectively remove aggregated or mutant rhodopsin from the cells and may be useful in treating RP associated with rhodopsin protein misfolding.

Published

2014

31. Druggable sensors of the unfolded protein response.

Author

Maly, Dustin J, Maly, Dustin J, Papa, Feroz R, Maly, Dustin J, Maly, Dustin J, and Papa, Feroz R

Abstract

The inability of cells to properly fold, modify and assemble secretory and transmembrane proteins leads to accumulation of misfolded proteins in the endoplasmic reticulum (ER). Under these conditions of 'ER stress', cell survival depends on homeostatic benefits from an intracellular signaling pathway called the unfolded protein response (UPR). When activated, the UPR induces transcriptional and translational programs that restore ER homeostasis. However, under high-level or chronic ER stress, these adaptive changes ultimately become overshadowed by alternative 'terminal UPR' signals that actively commit cells to degeneration, culminating in programmed cell death. Chronic ER stress and maladaptive UPR signaling are implicated in the etiology and pathogenesis of myriad human diseases. Naturally, this has generated widespread interest in targeting key nodal components of the UPR as therapeutic strategies. Here we summarize the state of this field with emphasis placed on two of the master UPR regulators, PERK and IRE1, which are both capable of being drugged with small molecules.

Published

2014

32. Systems biology. Conditional density-based analysis of T cell signaling in single-cell data.

Author

Krishnaswamy, Smita, Krishnaswamy, Smita, Spitzer, Matthew H, Mingueneau, Michael, Bendall, Sean C, Litvin, Oren, Stone, Erica, Pe'er, Dana, Nolan, Garry P, Krishnaswamy, Smita, Krishnaswamy, Smita, Spitzer, Matthew H, Mingueneau, Michael, Bendall, Sean C, Litvin, Oren, Stone, Erica, Pe'er, Dana, and Nolan, Garry P

Abstract

Cellular circuits sense the environment, process signals, and compute decisions using networks of interacting proteins. To model such a system, the abundance of each activated protein species can be described as a stochastic function of the abundance of other proteins. High-dimensional single-cell technologies, such as mass cytometry, offer an opportunity to characterize signaling circuit-wide. However, the challenge of developing and applying computational approaches to interpret such complex data remains. Here, we developed computational methods, based on established statistical concepts, to characterize signaling network relationships by quantifying the strengths of network edges and deriving signaling response functions. In comparing signaling between naïve and antigen-exposed CD4(+) T lymphocytes, we find that although these two cell subtypes had similarly wired networks, naïve cells transmitted more information along a key signaling cascade than did antigen-exposed cells. We validated our characterization on mice lacking the extracellular-regulated mitogen-activated protein kinase (MAPK) ERK2, which showed stronger influence of pERK on pS6 (phosphorylated-ribosomal protein S6), in naïve cells as compared with antigen-exposed cells, as predicted. We demonstrate that by using cell-to-cell variation inherent in single-cell data, we can derive response functions underlying molecular circuits and drive the understanding of how cells process signals.

Published

2014

33. Myxoma virus protein M029 is a dual function immunomodulator that inhibits PKR and also conscripts RHA/DHX9 to promote expanded host tropism and viral replication.

Author

Rahman, Masmudur M, Rahman, Masmudur M, Liu, Jia, Chan, Winnie M, Rothenburg, Stefan, McFadden, Grant, Rahman, Masmudur M, Rahman, Masmudur M, Liu, Jia, Chan, Winnie M, Rothenburg, Stefan, and McFadden, Grant

Abstract

Myxoma virus (MYXV)-encoded protein M029 is a member of the poxvirus E3 family of dsRNA-binding proteins that antagonize the cellular interferon signaling pathways. In order to investigate additional functions of M029, we have constructed a series of targeted M029-minus (vMyx-M029KO and vMyx-M029ID) and V5-tagged M029 MYXV. We found that M029 plays a pivotal role in determining the cellular tropism of MYXV in all mammalian cells tested. The M029-minus viruses were able to replicate only in engineered cell lines that stably express a complementing protein, such as vaccinia E3, but underwent abortive or abated infection in all other tested mammalian cell lines. The M029-minus viruses were dramatically attenuated in susceptible host European rabbits and caused no observable signs of myxomatosis. Using V5-tagged M029 virus, we observed that M029 expressed as an early viral protein is localized in both the nuclear and cytosolic compartments in virus-infected cells, and is also incorporated into virions. Using proteomic approaches, we have identified Protein Kinase R (PKR) and RNA helicase A (RHA)/DHX9 as two cellular binding partners of M029 protein. In virus-infected cells, M029 interacts with PKR in a dsRNA-dependent manner, while binding with DHX9 was not dependent on dsRNA. Significantly, PKR knockdown in human cells rescued the replication defect of the M029-knockout viruses. Unexpectedly, this rescue of M029-minus virus replication by PKR depletion could then be reversed by RHA/DHX9 knockdown in human monocytic THP1 cells. This indicates that M029 not only inhibits generic PKR anti-viral pathways, but also binds and conscripts RHA/DHX9 as a pro-viral effector to promote virus replication in THP1 cells. Thus, M029 is a critical host range and virulence factor for MYXV that is required for replication in all mammalian cells by antagonizing PKR-mediated anti-viral functions, and also conscripts pro-viral RHA/DHX9 to promote viral replication specifically in myeloid ce

Published

2013

34. Myxoma virus protein M029 is a dual function immunomodulator that inhibits PKR and also conscripts RHA/DHX9 to promote expanded host tropism and viral replication.

Author

Rahman, Masmudur M, Barry, Michele1, Rahman, Masmudur M, Liu, Jia, Chan, Winnie M, Rothenburg, Stefan, McFadden, Grant, Rahman, Masmudur M, Barry, Michele1, Rahman, Masmudur M, Liu, Jia, Chan, Winnie M, Rothenburg, Stefan, and McFadden, Grant

Abstract

Myxoma virus (MYXV)-encoded protein M029 is a member of the poxvirus E3 family of dsRNA-binding proteins that antagonize the cellular interferon signaling pathways. In order to investigate additional functions of M029, we have constructed a series of targeted M029-minus (vMyx-M029KO and vMyx-M029ID) and V5-tagged M029 MYXV. We found that M029 plays a pivotal role in determining the cellular tropism of MYXV in all mammalian cells tested. The M029-minus viruses were able to replicate only in engineered cell lines that stably express a complementing protein, such as vaccinia E3, but underwent abortive or abated infection in all other tested mammalian cell lines. The M029-minus viruses were dramatically attenuated in susceptible host European rabbits and caused no observable signs of myxomatosis. Using V5-tagged M029 virus, we observed that M029 expressed as an early viral protein is localized in both the nuclear and cytosolic compartments in virus-infected cells, and is also incorporated into virions. Using proteomic approaches, we have identified Protein Kinase R (PKR) and RNA helicase A (RHA)/DHX9 as two cellular binding partners of M029 protein. In virus-infected cells, M029 interacts with PKR in a dsRNA-dependent manner, while binding with DHX9 was not dependent on dsRNA. Significantly, PKR knockdown in human cells rescued the replication defect of the M029-knockout viruses. Unexpectedly, this rescue of M029-minus virus replication by PKR depletion could then be reversed by RHA/DHX9 knockdown in human monocytic THP1 cells. This indicates that M029 not only inhibits generic PKR anti-viral pathways, but also binds and conscripts RHA/DHX9 as a pro-viral effector to promote virus replication in THP1 cells. Thus, M029 is a critical host range and virulence factor for MYXV that is required for replication in all mammalian cells by antagonizing PKR-mediated anti-viral functions, and also conscripts pro-viral RHA/DHX9 to promote viral replication specifically in myeloid ce

Published

2013

35. Endoplasmic reticulum stress sensing in the unfolded protein response.

Author

Gardner, Brooke M, Gardner, Brooke M, Pincus, David, Gotthardt, Katja, Gallagher, Ciara M, Walter, Peter, Gardner, Brooke M, Gardner, Brooke M, Pincus, David, Gotthardt, Katja, Gallagher, Ciara M, and Walter, Peter

Abstract

Secretory and transmembrane proteins enter the endoplasmic reticulum (ER) as unfolded proteins and exit as either folded proteins in transit to their target organelles or as misfolded proteins targeted for degradation. The unfolded protein response (UPR) maintains the protein-folding homeostasis within the ER, ensuring that the protein-folding capacity of the ER meets the load of client proteins. Activation of the UPR depends on three ER stress sensor proteins, Ire1, PERK, and ATF6. Although the consequences of activation are well understood, how these sensors detect ER stress remains unclear. Recent evidence suggests that yeast Ire1 directly binds to unfolded proteins, which induces its oligomerization and activation. BiP dissociation from Ire1 regulates this oligomeric equilibrium, ultimately modulating Ire1's sensitivity and duration of activation. The mechanistic principles of ER stress sensing are the focus of this review.

Published

2013

36. Chemical genetics reveals a kinase-independent role for protein kinase R in pyroptosis.

Author

Hett, Erik C, Hett, Erik C, Slater, Louise H, Mark, Kevin G, Kawate, Tomohiko, Monks, Brian G, Stutz, Andrea, Latz, Eicke, Hung, Deborah T, Hett, Erik C, Hett, Erik C, Slater, Louise H, Mark, Kevin G, Kawate, Tomohiko, Monks, Brian G, Stutz, Andrea, Latz, Eicke, and Hung, Deborah T

Abstract

Formation of the inflammasome, a scaffolding complex that activates caspase-1, is important in numerous diseases. Pyroptotic cell death induced by anthrax lethal toxin (LT) is a model for inflammasome-mediated caspase-1 activation. We discovered 7-desacetoxy-6,7-dehydrogedunin (7DG) in a phenotypic screen as a small molecule that protects macrophages from LT-induced death. Using chemical proteomics, we identified protein kinase R (PKR) as the target of 7DG and show that RNAi knockdown of PKR phenocopies treatment with 7DG. Further, we show that PKR's role in ASC assembly and caspase-1 activation induced by several different inflammasome stimuli is independent of PKR's kinase activity, demonstrating that PKR has a previously uncharacterized role in caspase-1 activation and pyroptosis that is distinct from its reported kinase-dependent roles in apoptosis and inflammasome formation in lipopolysaccharide-primed cells. Remarkably, PKR has different roles in two distinct cell death pathways and has a broad role in inflammasome function relevant in other diseases.

Published

2013

37. Regulation of autophagy during ECM detachment is linked to a selective inhibition of mTORC1 by PERK.

Author

Aguirre-Ghiso, J, Aguirre-Ghiso, J, Avivar-Valderas, A, Bobrovnikova-Marjon, E, Alan Diehl, J, Bardeesy, N, Debnath, Jayanta, Aguirre-Ghiso, J, Aguirre-Ghiso, J, Avivar-Valderas, A, Bobrovnikova-Marjon, E, Alan Diehl, J, Bardeesy, N, and Debnath, Jayanta

Abstract

Adhesion to the extracellular matrix (ECM) is critical for epithelial tissue homeostasis and function. ECM detachment induces metabolic stress and programmed cell death via anoikis. ECM-detached mammary epithelial cells are able to rapidly activate autophagy allowing for survival and an opportunity for re-attachment. However, the mechanisms controlling detachment-induced autophagy remain unclear. Here we uncover that the kinase PERK rapidly promotes autophagy in ECM-detached cells by activating AMP-activated protein kinase (AMPK), resulting in downstream inhibition of mTORC1-p70(S6K) signaling. LKB1 and TSC2, but not TSC1, are required for PERK-mediated inhibition of mammalian target of rapamycinin MCF10A cells and mouse embryo fibroblast cells. Importantly, this pathway shows fast kinetics, is transcription-independent and is exclusively activated during ECM detachment, but not by canonical endoplasmic reticulum stressors. Moreover, enforced PERK or AMPK activation upregulates autophagy and causes luminal filling during acinar morphogenesis by perpetuating a population of surviving autophagic luminal cells that resist anoikis. Hence, we identify a novel pathway in which suspension-activated PERK promotes the activation of LKB1, AMPK and TSC2, leading to the rapid induction of detachment-induced autophagy. We propose that increased autophagy, secondary to persistent PERK and LKB1-AMPK signaling, can robustly protect cells from anoikis and promote luminal filling during early carcinoma progression.

Published

2013

38. Allelic methylation levels of the noncoding VTRNA2-1 located on chromosome 5q31.1 predict outcome in AML

Author

Treppendahl, Marianne Bach, Qiu, Xiangning, Søgaard, Alexandra, Yang, Xiaojing, Nandrup-Bus, Cecilie, Hother, Christoffer, Andersen, Mette Klarskov, Kjeldsen, Lars, Möllgård, Lars, Möllgaard, Lars, Hellström-Lindberg, Eva, Jendholm, Lars Johan, Porse, Bo T, Jones, Peter A, Liang, Gangning, Grønbæk, Kirsten, Treppendahl, Marianne Bach, Qiu, Xiangning, Søgaard, Alexandra, Yang, Xiaojing, Nandrup-Bus, Cecilie, Hother, Christoffer, Andersen, Mette Klarskov, Kjeldsen, Lars, Möllgård, Lars, Möllgaard, Lars, Hellström-Lindberg, Eva, Jendholm, Lars Johan, Porse, Bo T, Jones, Peter A, Liang, Gangning, and Grønbæk, Kirsten

Abstract

Deletions of chromosome 5q are associated with poor outcomes in acute myeloid leukemia (AML) suggesting the presence of tumor suppressor(s) at the locus. However, definitive identification of putative tumor suppressor genes remains controversial. Here we show that a 106-nucleotide noncoding RNA vault RNA2-1 (vtRNA2-1), previously misannotated as miR886, could potentially play a role in the biology and prognosis of AML. vtRNA2-1 is transcribed by polymerase III and is monoallelically methylated in 75% of healthy individuals whereas the remaining 25% of the population have biallelic hypomethylation. AML patients without methylation of VTRNA2-1 have a considerably better outcome than those with monoallelic or biallelic methylation (n = 101, P = .001). We show that methylation is inversely correlated with vtRNA2-1 expression, and that 5-azanucleosides induce vtRNA2-1 and down-regulate the phosphorylated RNA-dependent protein kinase (pPKR), whose activity has been shown to be modulated by vtRNA2-1. Because pPKR promotes cell survival in AML, the data are consistent with vtRNA2-1 being a tumor suppressor in AML. This is the first study to show that vtRNA2-1 might play a significant role in AML, that it is either mono- or biallelically expressed in the blood cells of healthy individuals, and that its methylation state predicts outcome in AML.

Published

2012

39. Allelic methylation levels of the noncoding VTRNA2-1 located on chromosome 5q31.1 predict outcome in AML

Author

Treppendahl, Marianne Bach, Qiu, Xiangning, Søgaard, Alexandra, Yang, Xiaojing, Nandrup-Bus, Cecilie, Hother, Christoffer, Andersen, Mette Klarskov, Kjeldsen, Lars, Möllgård, Lars, Möllgaard, Lars, Hellström-Lindberg, Eva, Jendholm, Lars Johan, Porse, Bo T, Jones, Peter A, Liang, Gangning, Grønbæk, Kirsten, Treppendahl, Marianne Bach, Qiu, Xiangning, Søgaard, Alexandra, Yang, Xiaojing, Nandrup-Bus, Cecilie, Hother, Christoffer, Andersen, Mette Klarskov, Kjeldsen, Lars, Möllgård, Lars, Möllgaard, Lars, Hellström-Lindberg, Eva, Jendholm, Lars Johan, Porse, Bo T, Jones, Peter A, Liang, Gangning, and Grønbæk, Kirsten

Abstract

Deletions of chromosome 5q are associated with poor outcomes in acute myeloid leukemia (AML) suggesting the presence of tumor suppressor(s) at the locus. However, definitive identification of putative tumor suppressor genes remains controversial. Here we show that a 106-nucleotide noncoding RNA vault RNA2-1 (vtRNA2-1), previously misannotated as miR886, could potentially play a role in the biology and prognosis of AML. vtRNA2-1 is transcribed by polymerase III and is monoallelically methylated in 75% of healthy individuals whereas the remaining 25% of the population have biallelic hypomethylation. AML patients without methylation of VTRNA2-1 have a considerably better outcome than those with monoallelic or biallelic methylation (n = 101, P = .001). We show that methylation is inversely correlated with vtRNA2-1 expression, and that 5-azanucleosides induce vtRNA2-1 and down-regulate the phosphorylated RNA-dependent protein kinase (pPKR), whose activity has been shown to be modulated by vtRNA2-1. Because pPKR promotes cell survival in AML, the data are consistent with vtRNA2-1 being a tumor suppressor in AML. This is the first study to show that vtRNA2-1 might play a significant role in AML, that it is either mono- or biallelically expressed in the blood cells of healthy individuals, and that its methylation state predicts outcome in AML.

Published

2012

40. Rapid evolution of protein kinase PKR alters sensitivity to viral inhibitors.

Author

Rothenburg, Stefan, Rothenburg, Stefan, Seo, Eun Joo, Gibbs, James S, Dever, Thomas E, Dittmar, Katharina, Rothenburg, Stefan, Rothenburg, Stefan, Seo, Eun Joo, Gibbs, James S, Dever, Thomas E, and Dittmar, Katharina

Abstract

Protein kinase PKR (also known as EIF2AK2) is activated during viral infection and phosphorylates the alpha subunit of eukaryotic translation initiation factor 2 (eIF2), leading to inhibition of translation and viral replication. We report fast evolution of the PKR kinase domain in vertebrates, coupled with positive selection of specific sites. Substitution of positively selected residues in human PKR with residues found in related species altered sensitivity to PKR inhibitors from different poxviruses. Species-specific differences in sensitivity to poxviral pseudosubstrate inhibitors were identified between human and mouse PKR, and these differences were traced to positively selected residues near the eIF2alpha binding site. Our findings indicate how an antiviral protein evolved to evade viral inhibition while maintaining its primary function. Moreover, the identified species-specific differences in the susceptibility to viral inhibitors have important implications for studying human infections in nonhuman model systems.

Published

2009

41. Divergent effects of PERK and IRE1 signaling on cell viability.

Author

Lin, Jonathan H, Lin, Jonathan H, Li, Han, Zhang, Yuhong, Ron, David, Walter, Peter, Lin, Jonathan H, Lin, Jonathan H, Li, Han, Zhang, Yuhong, Ron, David, and Walter, Peter

Abstract

Protein misfolding in the endoplasmic reticulum (ER) activates a set of intracellular signaling pathways, collectively termed the Unfolded Protein Response (UPR). UPR signaling promotes cell survival by reducing misfolded protein levels. If homeostasis cannot be restored, UPR signaling promotes cell death. The molecular basis for the switch between prosurvival and proapoptotic UPR function is poorly understood. The ER-resident proteins, PERK and IRE1, control two key UPR signaling pathways. Protein misfolding concomitantly activates PERK and IRE1 and has clouded insight into their contributions toward life or death cell fates. Here, we employed chemical-genetic strategies to activate individually PERK or IRE1 uncoupled from protein misfolding. We found that sustained PERK signaling impaired cell proliferation and promoted apoptosis. By contrast, equivalent durations of IRE1 signaling enhanced cell proliferation without promoting cell death. These results demonstrate that extended PERK and IRE1 signaling have opposite effects on cell viability. Differential activation of PERK and IRE1 may determine life or death decisions after ER protein misfolding.

Published

2009

42. Evidence of molecular links between PKR and mTOR signalling pathways in Abeta neurotoxicity: role of p53, Redd1 and TSC2.

Author

UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire, Morel, Milena, Couturier, Julien, Pontcharraud, Raymond, Gil, Roger, Fauconneau, Bernard, Paccalin, Marc, Page, Guylène, UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire, Morel, Milena, Couturier, Julien, Pontcharraud, Raymond, Gil, Roger, Fauconneau, Bernard, Paccalin, Marc, and Page, Guylène

Abstract

The control of translation is disturbed in Alzheimer's disease (AD). This study analysed the crosslink between the up regulation of double-stranded RNA-dependent-protein kinase (PKR) and the down regulation of mammalian target of rapamycin (mTOR) signalling pathways via p53, the protein Regulated in the Development and DNA damage response 1 (Redd1) and the tuberous sclerosis complex (TSC2) factors in two beta-amyloid peptide (Abeta) neurotoxicity models. In SH-SY5Y cells, Abeta42 induced an increase of P(T451)-PKR and of the ratio p66/(p66+p53) in nuclei and a physical interaction between these proteins. Redd1 gene levels increased and P(T1462)-TSC2 decreased. These disturbances were earlier in rat primary neurons with nuclear co-localization of Redd1 and PKR. The PKR gene silencing in SH-SY5Y cells prevented these alterations. p53, Redd1 and TSC2 could represent the molecular links between PKR and mTOR in Abeta neurotoxicity. PKR could be a critical target in a therapeutic program of AD.

Published

2009

43. PKR, the double stranded RNA-dependent protein kinase as a critical target in Alzheimer's disease.

Author

University of Poitiers - Research Group on Brain Aging (EA 3808), Morel, Milena, Couturier, Julien, Lafay-Chebassier, Claire, Paccalin, Marc, Page, Guylène, University of Poitiers - Research Group on Brain Aging (EA 3808), Morel, Milena, Couturier, Julien, Lafay-Chebassier, Claire, Paccalin, Marc, and Page, Guylène

Abstract

Amyloid beta-peptide (Abeta) deposits and neurofibrillary tangles are key hallmarks in Alzheimer's disease (AD). Abeta stimulates many signal transducers involved in the neuronal death. However, many mechanisms remain to be elucidated because no definitive therapy of AD exists. Some studies have focused on the control of translation which involves eIF2 and eIF4E, main eukaryotic factors of initiation. The availability of these factors depends on the activation of the double-stranded RNA-dependent protein kinase (PKR) and the mammalian target of rapamycin (mTOR), respectively. mTOR positively regulates the translation while PKR results in a protein synthesis shutdown. Many studies demonstrated that the PKR signalling pathway is up-regulated in cellular and animal models of AD and in the brain of AD patients. Interestingly, our results showed that phosphorylated PKR and eIF2alpha levels were significantly increased in lymphocytes of AD patients. These modifications were significantly correlated with cognitive and memory test scores performed in AD patients. On the contrary, the mTOR signalling pathway is down-regulated in cellular and animal models of AD. Recently, we showed that p53, regulated protein in development and DNA damage response 1 and tuberous sclerosis complex 2 could represent molecular links between PKR and mTOR signalling pathways. PKR could be an early biomarker of the neuronal death and a critical target for a therapeutic programme in AD.

Published

2009

44. Divergent effects of PERK and IRE1 signaling on cell viability.

Author

Lin, Jonathan H, Bergmann, Andreas1, Lin, Jonathan H, Li, Han, Zhang, Yuhong, Ron, David, Walter, Peter, Lin, Jonathan H, Bergmann, Andreas1, Lin, Jonathan H, Li, Han, Zhang, Yuhong, Ron, David, and Walter, Peter

Abstract

Protein misfolding in the endoplasmic reticulum (ER) activates a set of intracellular signaling pathways, collectively termed the Unfolded Protein Response (UPR). UPR signaling promotes cell survival by reducing misfolded protein levels. If homeostasis cannot be restored, UPR signaling promotes cell death. The molecular basis for the switch between prosurvival and proapoptotic UPR function is poorly understood. The ER-resident proteins, PERK and IRE1, control two key UPR signaling pathways. Protein misfolding concomitantly activates PERK and IRE1 and has clouded insight into their contributions toward life or death cell fates. Here, we employed chemical-genetic strategies to activate individually PERK or IRE1 uncoupled from protein misfolding. We found that sustained PERK signaling impaired cell proliferation and promoted apoptosis. By contrast, equivalent durations of IRE1 signaling enhanced cell proliferation without promoting cell death. These results demonstrate that extended PERK and IRE1 signaling have opposite effects on cell viability. Differential activation of PERK and IRE1 may determine life or death decisions after ER protein misfolding.

Published

2009

45. Rapid evolution of protein kinase PKR alters sensitivity to viral inhibitors.

Author

Rothenburg, Stefan, Rothenburg, Stefan, Seo, Eun Joo, Gibbs, James S, Dever, Thomas E, Dittmar, Katharina, Rothenburg, Stefan, Rothenburg, Stefan, Seo, Eun Joo, Gibbs, James S, Dever, Thomas E, and Dittmar, Katharina

Abstract

Protein kinase PKR (also known as EIF2AK2) is activated during viral infection and phosphorylates the alpha subunit of eukaryotic translation initiation factor 2 (eIF2), leading to inhibition of translation and viral replication. We report fast evolution of the PKR kinase domain in vertebrates, coupled with positive selection of specific sites. Substitution of positively selected residues in human PKR with residues found in related species altered sensitivity to PKR inhibitors from different poxviruses. Species-specific differences in sensitivity to poxviral pseudosubstrate inhibitors were identified between human and mouse PKR, and these differences were traced to positively selected residues near the eIF2alpha binding site. Our findings indicate how an antiviral protein evolved to evade viral inhibition while maintaining its primary function. Moreover, the identified species-specific differences in the susceptibility to viral inhibitors have important implications for studying human infections in nonhuman model systems.

Published

2009

46. c-Jun NH2-terminal kinase activity in subcutaneous adipose tissue but not nuclear factor-kappaB activity in peripheral blood mononuclear cells is an independent determinant of insulin resistance in healthy individuals

Author

Sourris, Karly C, Lyons, Jasmine G, de Courten, Maximilian, Dougherty, Sonia L, Henstridge, Darren C, Cooper, Mark E, Hage, Michelle, Dart, Anthony, Kingwell, Bronwyn A, Forbes, Josephine M, de Courten, Barbora, Sourris, Karly C, Lyons, Jasmine G, de Courten, Maximilian, Dougherty, Sonia L, Henstridge, Darren C, Cooper, Mark E, Hage, Michelle, Dart, Anthony, Kingwell, Bronwyn A, Forbes, Josephine M, and de Courten, Barbora

Abstract

Chronic low-grade activation of the immune system (CLAIS) predicts type 2 diabetes via a decrease in insulin sensitivity. Our study investigated potential relationships between nuclear factor-kappaB (NF-kappaB) and c-Jun NH(2)-terminal kinase (JNK) pathways-two pathways proposed as the link between CLAIS and insulin resistance.

Published

2009

47. c-Jun NH2-terminal kinase activity in subcutaneous adipose tissue but not nuclear factor-kappaB activity in peripheral blood mononuclear cells is an independent determinant of insulin resistance in healthy individuals

Author

Sourris, Karly C, Lyons, Jasmine G, de Courten, Maximilian, Dougherty, Sonia L, Henstridge, Darren C, Cooper, Mark E, Hage, Michelle, Dart, Anthony, Kingwell, Bronwyn A, Forbes, Josephine M, de Courten, Barbora, Sourris, Karly C, Lyons, Jasmine G, de Courten, Maximilian, Dougherty, Sonia L, Henstridge, Darren C, Cooper, Mark E, Hage, Michelle, Dart, Anthony, Kingwell, Bronwyn A, Forbes, Josephine M, and de Courten, Barbora

Abstract

Chronic low-grade activation of the immune system (CLAIS) predicts type 2 diabetes via a decrease in insulin sensitivity. Our study investigated potential relationships between nuclear factor-kappaB (NF-kappaB) and c-Jun NH(2)-terminal kinase (JNK) pathways-two pathways proposed as the link between CLAIS and insulin resistance.

Published

2009

48. Initiation and execution of lipotoxic ER stress in pancreatic beta-cells.

Author

Andrade Da Cunha, Daniel, Hekerman, Paul, Ladrière, Laurence, Bazarra-Castro, A., Ortis, Fernanda, Wakeham, Marion, Moore, Fabrice, Rasschaert, Joanne, Cardozo, Alessandra K, Bellomo, Elisa, Overbergh, Lutgart, Mathieu, Chantal, Lupi, R., Hai, Tsonwin, Herchuelz, André, Marchetti, Piero, Rutter, Guy A, Eizirik, Decio L., Cnop, Miriam, Andrade Da Cunha, Daniel, Hekerman, Paul, Ladrière, Laurence, Bazarra-Castro, A., Ortis, Fernanda, Wakeham, Marion, Moore, Fabrice, Rasschaert, Joanne, Cardozo, Alessandra K, Bellomo, Elisa, Overbergh, Lutgart, Mathieu, Chantal, Lupi, R., Hai, Tsonwin, Herchuelz, André, Marchetti, Piero, Rutter, Guy A, Eizirik, Decio L., and Cnop, Miriam

Abstract

Free fatty acids (FFA) cause apoptosis of pancreatic beta-cells and might contribute to beta-cell loss in type 2 diabetes via the induction of endoplasmic reticulum (ER) stress. We studied here the molecular mechanisms implicated in FFA-induced ER stress initiation and apoptosis in INS-1E cells, FACS-purified primary beta-cells and human islets exposed to oleate and/or palmitate. Treatment with saturated and/or unsaturated FFA led to differential ER stress signaling. Palmitate induced more apoptosis and markedly activated the IRE1, PERK and ATF6 pathways, owing to a sustained depletion of ER Ca(2+) stores, whereas the unsaturated FFA oleate led to milder PERK and IRE1 activation and comparable ATF6 signaling. Non-metabolizable methyl-FFA analogs induced neither ER stress nor beta-cell apoptosis. The FFA-induced ER stress response was not modified by high glucose concentrations, suggesting that ER stress in primary beta-cells is primarily lipotoxic, and not glucolipotoxic. Palmitate, but not oleate, activated JNK. JNK inhibitors reduced palmitate-mediated AP-1 activation and apoptosis. Blocking the transcription factor CHOP delayed palmitate-induced beta-cell apoptosis. In conclusion, saturated FFA induce ER stress via ER Ca(2+) depletion. The IRE1 and resulting JNK activation contribute to beta-cell apoptosis. PERK activation by palmitate also contributes to beta-cell apoptosis via CHOP., Journal Article, Research Support, N.I.H. Extramural, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2008

49. Double-stranded RNA-activated protein kinase PKR of fishes and amphibians: varying the number of double-stranded RNA binding domains and lineage-specific duplications.

Author

Rothenburg, Stefan, Rothenburg, Stefan, Deigendesch, Nikolaus, Dey, Madhusudan, Dever, Thomas E, Tazi, Loubna, Rothenburg, Stefan, Rothenburg, Stefan, Deigendesch, Nikolaus, Dey, Madhusudan, Dever, Thomas E, and Tazi, Loubna

Abstract

BackgroundDouble-stranded (ds) RNA, generated during viral infection, binds and activates the mammalian anti-viral protein kinase PKR, which phosphorylates the translation initiation factor eIF2alpha leading to the general inhibition of protein synthesis. Although PKR-like activity has been described in fish cells, the responsible enzymes eluded molecular characterization until the recent discovery of goldfish and zebrafish PKZ, which contain Z-DNA-binding domains instead of dsRNA-binding domains (dsRBDs). Fish and amphibian PKR genes have not been described so far.ResultsHere we report the cloning and identification of 13 PKR genes from 8 teleost fish and amphibian species, including zebrafish, demonstrating the coexistence of PKR and PKZ in this latter species. Analyses of their genomic organization revealed up to three tandemly arrayed PKR genes, which are arranged in head-to-tail orientation. At least five duplications occurred independently in fish and amphibian lineages. Phylogenetic analyses reveal that the kinase domains of fish PKR genes are more closely related to those of fish PKZ than to the PKR kinase domains of other vertebrate species. The duplication leading to fish PKR and PKZ genes occurred early during teleost fish evolution after the divergence of the tetrapod lineage. While two dsRBDs are found in mammalian and amphibian PKR, one, two or three dsRBDs are present in fish PKR. In zebrafish, both PKR and PKZ were strongly upregulated after immunostimulation with some tissue-specific expression differences. Using genetic and biochemical assays we demonstrate that both zebrafish PKR and PKZ can phosphorylate eIF2alpha in yeast.ConclusionConsidering the important role for PKR in host defense against viruses, the independent duplication and fixation of PKR genes in different lineages probably provided selective advantages by leading to the recognition of an extended spectrum of viral nucleic acid structures, including both dsRNA and Z-DNA/RNA, and perh

Published

2008

50. Double-stranded RNA-activated protein kinase PKR of fishes and amphibians: varying the number of double-stranded RNA binding domains and lineage-specific duplications.

Author

Rothenburg, Stefan, Rothenburg, Stefan, Deigendesch, Nikolaus, Dey, Madhusudan, Dever, Thomas E, Tazi, Loubna, Rothenburg, Stefan, Rothenburg, Stefan, Deigendesch, Nikolaus, Dey, Madhusudan, Dever, Thomas E, and Tazi, Loubna

Abstract

BackgroundDouble-stranded (ds) RNA, generated during viral infection, binds and activates the mammalian anti-viral protein kinase PKR, which phosphorylates the translation initiation factor eIF2alpha leading to the general inhibition of protein synthesis. Although PKR-like activity has been described in fish cells, the responsible enzymes eluded molecular characterization until the recent discovery of goldfish and zebrafish PKZ, which contain Z-DNA-binding domains instead of dsRNA-binding domains (dsRBDs). Fish and amphibian PKR genes have not been described so far.ResultsHere we report the cloning and identification of 13 PKR genes from 8 teleost fish and amphibian species, including zebrafish, demonstrating the coexistence of PKR and PKZ in this latter species. Analyses of their genomic organization revealed up to three tandemly arrayed PKR genes, which are arranged in head-to-tail orientation. At least five duplications occurred independently in fish and amphibian lineages. Phylogenetic analyses reveal that the kinase domains of fish PKR genes are more closely related to those of fish PKZ than to the PKR kinase domains of other vertebrate species. The duplication leading to fish PKR and PKZ genes occurred early during teleost fish evolution after the divergence of the tetrapod lineage. While two dsRBDs are found in mammalian and amphibian PKR, one, two or three dsRBDs are present in fish PKR. In zebrafish, both PKR and PKZ were strongly upregulated after immunostimulation with some tissue-specific expression differences. Using genetic and biochemical assays we demonstrate that both zebrafish PKR and PKZ can phosphorylate eIF2alpha in yeast.ConclusionConsidering the important role for PKR in host defense against viruses, the independent duplication and fixation of PKR genes in different lineages probably provided selective advantages by leading to the recognition of an extended spectrum of viral nucleic acid structures, including both dsRNA and Z-DNA/RNA, and perh

Published

2008