Your search keyword '"Shai B"' showing total 116 results

101. ATF3 Regulates the Expression of AChE During Stress

Author

Ronit Heinrich, Rivka Hertz, Esther Zemel, Irit Mann, Liat Brenner, Amir Massarweh, Shai Berlin, and Ido Perlman

Subjects

retina, ATF3, AChE, degeneration, photic stress, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Acetylcholinesterase (AChE) expresses in non-cholinergic cells, but its role(s) there remain unknown. We have previously attributed a pro-apoptotic role for AChE in stressed retinal photoreceptors, though by unknown mechanism. Here, we examined its promoter only to find that it includes a binding sequence for the activating transcription factor 3 (ATF3); a prototypical mediator of apoptosis. This suggests that expression of AChE could be regulated by ATF3 in the retina. Indeed, ATF3 binds the AChE-promoter to down-regulate its expressions in vitro. Strikingly, retinas of “blinded” mice display hallmarks of apoptosis, almost exclusively in the outer nuclear layer (ONL); coinciding with elevated levels of AChE and absence of ATF3. A mirror image is observed in the inner nuclear layer (INL), namely prominent levels of ATF3 and lack of AChE as well as lack of apoptosis. We conclude that segregated patterns of expressions of ATF3 reflect its ability to repress apoptosis in different layers of the retina—a novel mechanism behind apoptosis.

Published

2018

102. Israeli Theatre in 2017: Visions of a Cleft Heart

Author

Shai Bar Yaacov

Subjects

Dramatic representation. The theater, PN2000-3307

Published

2017

103. Clinical Trials of Exterior Non Implanted Interference-Based Extended Depth of Focus Intra Ocular Lens Design

Author

Zeev Zalevsky, Ido Raveh, Ofer Limon, Shai Ben Yaish, Karen Lahav Yacouel, Ravid Doron, and Alex Zlotnik

Subjects

extended depth of focus, intra ocular lenses, cataract surgery, Applied optics. Photonics, TA1501-1820

Abstract

In this paper, we present the clinical trials performed with intra ocular lens (IOL) design, realizing an interference-based extended depth of focus concept, with an external glass plate. The purpose of such extended depth of focus-based IOL design is to prevent cataract patients from needing to use different types of glasses (for reading and for distance vision) after undergoing surgery.

Published

2014

104. A family of photoswitchable NMDA receptors

Author

Shai Berlin, Stephanie Szobota, Andreas Reiner, Elizabeth C Carroll, Michael A Kienzler, Alice Guyon, Tong Xiao, Dirk Trauner, and Ehud Y Isacoff

Subjects

NMDA receptor, photoswitch, LiGluN, GluN2, synaptic plasticity, synapse, Medicine, Science, Biology (General), QH301-705.5

Abstract

NMDA receptors, which regulate synaptic strength and are implicated in learning and memory, consist of several subtypes with distinct subunit compositions and functional properties. To enable spatiotemporally defined, rapid and reproducible manipulation of function of specific subtypes, we engineered a set of photoswitchable GluN subunits ('LiGluNs'). Photo-agonism of GluN2A or GluN2B elicits an excitatory drive to hippocampal neurons that can be shaped in time to mimic synaptic activation. Photo-agonism of GluN2A at single dendritic spines evokes spine-specific calcium elevation and expansion, the morphological correlate of LTP. Photo-antagonism of GluN2A alone, or in combination with photo-antagonism of GluN1a, reversibly blocks excitatory synaptic currents, prevents the induction of long-term potentiation and prevents spine expansion. In addition, photo-antagonism in vivo disrupts synaptic pruning of developing retino-tectal projections in larval zebrafish. By providing precise and rapidly reversible optical control of NMDA receptor subtypes, LiGluNs should help unravel the contribution of specific NMDA receptors to synaptic transmission, integration and plasticity.

Published

2016

105. A Quantitative Model of the GIRK1/2 Channel Reveals That Its Basal and Evoked Activities Are Controlled by Unequal Stoichiometry of Gα and Gβγ.

Author

Daniel Yakubovich, Shai Berlin, Uri Kahanovitch, Moran Rubinstein, Isabella Farhy-Tselnicker, Boaz Styr, Tal Keren-Raifman, Carmen W Dessauer, and Nathan Dascal

Subjects

Biology (General), QH301-705.5

Abstract

G protein-gated K+ channels (GIRK; Kir3), activated by Gβγ subunits derived from Gi/o proteins, regulate heartbeat and neuronal excitability and plasticity. Both neurotransmitter-evoked (Ievoked) and neurotransmitter-independent basal (Ibasal) GIRK activities are physiologically important, but mechanisms of Ibasal and its relation to Ievoked are unclear. We have previously shown for heterologously expressed neuronal GIRK1/2, and now show for native GIRK in hippocampal neurons, that Ibasal and Ievoked are interrelated: the extent of activation by neurotransmitter (activation index, Ra) is inversely related to Ibasal. To unveil the underlying mechanisms, we have developed a quantitative model of GIRK1/2 function. We characterized single-channel and macroscopic GIRK1/2 currents, and surface densities of GIRK1/2 and Gβγ expressed in Xenopus oocytes. Based on experimental results, we constructed a mathematical model of GIRK1/2 activity under steady-state conditions before and after activation by neurotransmitter. Our model accurately recapitulates Ibasal and Ievoked in Xenopus oocytes, HEK293 cells and hippocampal neurons; correctly predicts the dose-dependent activation of GIRK1/2 by coexpressed Gβγ and fully accounts for the inverse Ibasal-Ra correlation. Modeling indicates that, under all conditions and at different channel expression levels, between 3 and 4 Gβγ dimers are available for each GIRK1/2 channel. In contrast, available Gαi/o decreases from ~2 to less than one Gα per channel as GIRK1/2's density increases. The persistent Gβγ/channel (but not Gα/channel) ratio support a strong association of GIRK1/2 with Gβγ, consistent with recruitment to the cell surface of Gβγ, but not Gα, by GIRK1/2. Our analysis suggests a maximal stoichiometry of 4 Gβγ but only 2 Gαi/o per one GIRK1/2 channel. The unique, unequal association of GIRK1/2 with G protein subunits, and the cooperative nature of GIRK gating by Gβγ, underlie the complex pattern of basal and agonist-evoked activities and allow GIRK1/2 to act as a sensitive bidirectional detector of both Gβγ and Gα.

Published

2015

106. TMF/ARA160 Governs the Dynamic Spatial Orientation of the Golgi Apparatus during Sperm Development.

Author

Yoav Elkis, Shai Bel, Roni Rahimi, Tali Lerer-Goldstein, Smadar Levin-Zaidman, Tatiana Babushkin, Sally Shpungin, and Uri Nir

Subjects

Medicine, Science

Abstract

TMF/ARA160 is known to be a TATA element Modulatory Factor (TMF). It was initially identified as a DNA-binding factor and a coactivator of the Androgen receptor. It was also characterized as a Golgi-associated protein, which is essential for acrosome formation during functional sperm development. However, the molecular roles of TMF in this intricate process have not been revealed. Here, we show that during spermiogenesis, TMF undergoes a dynamic change of localization throughout the Golgi apparatus. Specifically, TMF translocates from the cis-Golgi to the trans-Golgi network and to the emerging vesicles surface, as the round spermatids develop. Notably, lack of TMF led to an abnormal spatial orientation of the Golgi and to the deviation of the trans-Golgi surface away from the nucleus of the developing round spermatids. Concomitantly, pro-acrosomal vesicles derived from the TMF-/- Golgi lacked targeting properties and did not tether to the spermatid nuclear membrane thereby failing to form the acrosome anchoring scaffold, the acroplaxome, around the cell-nucleus. Absence of TMF also perturbed the positioning of microtubules, which normally lie in proximity to the Golgi and are important for maintaining Golgi spatial orientation and dynamics and for chromatoid body formation, which is impaired in TMF-/- spermatids. In-silico evaluation combined with molecular and electron microscopic analyses revealed the presence of a microtubule interacting domain (MIT) in TMF, and confirmed the association of TMF with microtubules in spermatogenic cells. Furthermore, the MIT domain in TMF, along with microtubules integrity, are required for stable association of TMF with the Golgi apparatus. Collectively, we show here for the first time that a Golgi and microtubules associated protein is crucial for maintaining proper Golgi orientation during a cell developmental process.

Published

2015

107. The Eps1p protein disulfide isomerase conserves classic thioredoxin superfamily amino acid motifs but not their functional geometries.

Author

Shai Biran, Yair Gat, and Deborah Fass

Subjects

Medicine, Science

Abstract

The widespread thioredoxin superfamily enzymes typically share the following features: a characteristic α-β fold, the presence of a Cys-X-X-Cys (or Cys-X-X-Ser) redox-active motif, and a proline in the cis configuration abutting the redox-active site in the tertiary structure. The Cys-X-X-Cys motif is at the solvent-exposed amino terminus of an α-helix, allowing the first cysteine to engage in nucleophilic attack on substrates, or substrates to attack the Cys-X-X-Cys disulfide, depending on whether the enzyme functions to reduce, isomerize, or oxidize its targets. We report here the X-ray crystal structure of an enzyme that breaks many of our assumptions regarding the sequence-structure relationship of thioredoxin superfamily proteins. The yeast Protein Disulfide Isomerase family member Eps1p has Cys-X-X-Cys motifs and proline residues at the appropriate primary structural positions in its first two predicted thioredoxin-fold domains. However, crystal structures show that the Cys-X-X-Cys of the second domain is buried and that the adjacent proline is in the trans, rather than the cis isomer. In these configurations, neither the "active-site" disulfide nor the backbone carbonyl preceding the proline is available to interact with substrate. The Eps1p structures thus expand the documented diversity of the PDI oxidoreductase family and demonstrate that conserved sequence motifs in common folds do not guarantee structural or functional conservation.

Published

2014

108. Photonic RF-IF wideband down conversion using optical injection locking

Author

George, Thomas, Dutta, Achyut K., Islam, M. Saif, Adleman, James R., Lin, Chunyan L., Jester, Shai B., Pascoguin, B. M., Evans, Douglass C., and Jacobs, Everett W.

Published

2015

109. It does exist! A left-to-right spatial-numerical association of response codes (SNARC) effect among native Hebrew speakers.

Author

Zohar-Shai B, Tzelgov J, Karni A, and Rubinsten O

Subjects

Adult, Female, Humans, Israel, Male, Young Adult, Mathematical Concepts, Psycholinguistics, Reading, Space Perception physiology

Abstract

Several studies, starting with Dehaene, Bossini, and Giraux (1993), have reported that, in parity-judgment tasks, the difference in response latencies generated by the right and left hand are negatively correlated with number magnitudes. This SNARC (spatial-numerical association of response codes) effect is in line with the notion that the "mental number line" extends from left to right. The SNARC effect has been found mainly in native speakers of Germanic/Romanic languages; it has been suggested that the SNARC effect may derive from the experience of reading from left to right. To date, there is no evidence that the SNARC (or reverse SNARC) effect exists in parity judgments in native speakers of Hebrew readers. Here we provide the first demonstration of a horizontal, left-to-right SNARC effect in native speakers of Hebrew performing the parity task. Although we found no SNARC effect using the standard parity task, a reliable SNARC effect was found when we succeeded in reducing the MARC (markedness association of response codes) effect. We succeeded in reducing the MARC effect by implementing the parity task in 2 sessions, on 2 different days, each time using a different mapping of the parity-to-response side. (PsycINFO Database Record, ((c) 2017 APA, all rights reserved).)

Published

2017

110. Combined genetic and epigenetic interferences with interferon signaling expose prostate cancer cells to viral infection.

Author

Danziger O, Shai B, Sabo Y, Bacharach E, and Ehrlich M

Subjects

Cell Line, Tumor, Epigenesis, Genetic, Humans, Janus Kinase 1 metabolism, Male, Gene Expression Regulation, Neoplastic genetics, Interferons metabolism, Oncolytic Virotherapy, Prostatic Neoplasms genetics, Signal Transduction physiology

Abstract

Interferons (IFNs) induce anti-viral programs, regulate immune responses, and exert anti-proliferative effects. To escape anti-tumorigenic effects of IFNs, malignant cells attenuate JAK/STAT signaling and expression of IFN stimulated genes (ISGs). Such attenuation may enhance the susceptibility of tumor cells to oncolytic virotherapy. Here we studied genetic and epigenetic mechanisms of interference with JAK/STAT signaling and their contribution to susceptibility of prostate cancer cells to viral infection. Bioinformatics analysis of gene-expression in cohorts of prostate cancer patients revealed genetic and epigenetic interference with the IFN program. To correlate lack of IFN signaling and susceptibility to viral infection and oncolysis; we employed LNCaP prostate cancer cells as cellular model, and the human metapneumovirus and the epizootic hemorrhagic disease virus as infectious agents. In LNCaP cells, JAK1 is silenced by bi-allelic inactivating mutations and epigenetic silencing, which also silences ISGs. Chemical inhibition of epigenetic silencing partially restored IFN-sensitivity, induced low levels of expression of selected ISGs and attenuated, but failed to block, viral infection and oncolysis. Since viral infection was not blocked by epigenetic modifiers, and these compounds may independently-induce anti-tumor effects, we propose that epigenetic modifiers and virotherapy are compatible in treatment of prostate tumors defective in JAK1 expression and IFN signaling., Competing Interests: We declare no potential conflicts of interest.

Published

2016

111. The glucosinolate breakdown product indole-3-carbinol acts as an auxin antagonist in roots of Arabidopsis thaliana.

Author

Katz E, Nisani S, Yadav BS, Woldemariam MG, Shai B, Obolski U, Ehrlich M, Shani E, Jander G, and Chamovitz DA

Subjects

Arabidopsis Proteins metabolism, Gene Expression Regulation, Plant drug effects, Indoleacetic Acids antagonists & inhibitors, Arabidopsis drug effects, Arabidopsis metabolism, Glucosinolates metabolism, Indoles metabolism, Indoles pharmacology, Plant Roots drug effects, Plant Roots metabolism

Abstract

The glucosinolate breakdown product indole-3-carbinol functions in cruciferous vegetables as a protective agent against foraging insects. While the toxic and deterrent effects of glucosinolate breakdown on herbivores and pathogens have been studied extensively, the secondary responses that are induced in the plant by indole-3-carbinol remain relatively uninvestigated. Here we examined the hypothesis that indole-3-carbinol plays a role in influencing plant growth and development by manipulating auxin signaling. We show that indole-3-carbinol rapidly and reversibly inhibits root elongation in a dose-dependent manner, and that this inhibition is accompanied by a loss of auxin activity in the root meristem. A direct interaction between indole-3-carbinol and the auxin perception machinery was suggested, as application of indole-3-carbinol rescues auxin-induced root phenotypes. In vitro and yeast-based protein interaction studies showed that indole-3-carbinol perturbs the auxin-dependent interaction of Transport Inhibitor Response (TIR1) with auxin/3-indoleacetic acid (Aux/IAAs) proteins, further supporting the possibility that indole-3-carbinol acts as an auxin antagonist. The results indicate that chemicals whose production is induced by herbivory, such as indole-3-carbinol, function not only to repel herbivores, but also as signaling molecules that directly compete with auxin to fine tune plant growth and development., (© 2015 The Authors The Plant Journal © 2015 John Wiley & Sons Ltd.)

Published

2015

112. Mammalian ER mannosidase I resides in quality control vesicles, where it encounters its glycoprotein substrates.

Author

Benyair R, Ogen-Shtern N, Mazkereth N, Shai B, Ehrlich M, and Lederkremer GZ

Subjects

Animals, Autophagy, Endoplasmic Reticulum Stress, Endoplasmic Reticulum-Associated Degradation, Fluorescence Resonance Energy Transfer, HEK293 Cells, HeLa Cells, Humans, Immunoblotting, Luminescent Proteins genetics, Luminescent Proteins metabolism, Mannosidases genetics, Mice, Microscopy, Confocal, Microtubule-Associated Proteins genetics, Microtubule-Associated Proteins metabolism, Microtubules metabolism, NIH 3T3 Cells, Substrate Specificity, Time-Lapse Imaging methods, Cytoplasmic Vesicles metabolism, Endoplasmic Reticulum enzymology, Glycoproteins metabolism, Mannosidases metabolism

Abstract

Endoplasmic reticulum α1,2 mannosidase I (ERManI), a central component of ER quality control and ER-associated degradation (ERAD), acts as a timer enzyme, modifying N-linked sugar chains of glycoproteins with time. This process halts glycoprotein folding attempts when necessary and targets terminally misfolded glycoproteins to ERAD. Despite the importance of ERManI in maintenance of glycoprotein quality control, fundamental questions regarding this enzyme remain controversial. One such question is the subcellular localization of ERManI, which has been suggested to localize to the ER membrane, the ER-derived quality control compartment (ERQC), and, surprisingly, recently to the Golgi apparatus. To try to clarify this controversy, we applied a series of approaches that indicate that ERManI is located, at the steady state, in quality control vesicles (QCVs) to which ERAD substrates are transported and in which they interact with the enzyme. Both endogenous and exogenously expressed ERManI migrate at an ER-like density on iodixanol gradients, suggesting that the QCVs are derived from the ER. The QCVs are highly mobile, displaying dynamics that are dependent on microtubules and COP-II but not on COP-I vesicle machinery. Under ER stress conditions, the QCVs converge in a juxtanuclear region, at the ERQC, as previously reported. Our results also suggest that ERManI is turned over by an active autophagic process. Of importance, we found that membrane disturbance, as is common in immunofluorescence methods, leads to an artificial appearance of ERManI in a Golgi pattern., (© 2015 Benyair et al. This article is distributed by The American Society for Cell Biology under license from the author(s). Two months after publication it is available to the public under an Attribution–Noncommercial–Share Alike 3.0 Unported Creative Commons License (http://creativecommons.org/licenses/by-nc-sa/3.0).)

Published

2015

113. Epizootic hemorrhagic disease virus induces and benefits from cell stress, autophagy, and apoptosis.

Author

Shai B, Schmukler E, Yaniv R, Ziv N, Horn G, Bumbarov V, Yadin H, Smorodinsky NI, Bacharach E, Pinkas-Kramarski R, and Ehrlich M

Subjects

Animals, Cattle, Cattle Diseases genetics, Cattle Diseases metabolism, Cattle Diseases virology, Cell Line, Hemorrhagic Disease Virus, Epizootic genetics, MAP Kinase Kinase 4 genetics, MAP Kinase Kinase 4 metabolism, Mice, Protein Biosynthesis, Proto-Oncogene Proteins c-jun genetics, Proto-Oncogene Proteins c-jun metabolism, Reoviridae Infections metabolism, Reoviridae Infections physiopathology, Reoviridae Infections virology, Sheep, Sheep Diseases genetics, Sheep Diseases metabolism, Sheep Diseases virology, Signal Transduction, Apoptosis, Autophagy, Cattle Diseases physiopathology, Hemorrhagic Disease Virus, Epizootic physiology, Reoviridae Infections veterinary, Sheep Diseases physiopathology

Abstract

The mode and timing of virally induced cell death hold the potential of regulating viral yield, viral transmission, and the severity of virally induced disease. Orbiviruses such as the epizootic hemorrhagic disease virus (EHDV) are nonenveloped and cytolytic. To date, the death of cells infected with EHDV, the signal transduction pathways involved in this process, and the consequence of their inhibition have yet to be characterized. Here, we report that the Ibaraki strain of EHDV2 (EHDV2-IBA) induces apoptosis, autophagy, a decrease in cellular protein synthesis, the activation of c-Jun N-terminal kinase (JNK), and the phosphorylation of the JNK substrate c-Jun. The production of infectious virions decreased upon inhibition of apoptosis with the pan-caspase inhibitor Q-VD-OPH (quinolyl-valyl-O-methylaspartyl-[-2,6-difluorophenoxy]-methyl ketone), upon inhibition of autophagy with 3-methyladenine or via the knockout of the autophagy regulator Atg5, or upon treatment of infected cells with the JNK inhibitor SP600125 or the cyclin-dependent kinase (CDK) inhibitor roscovitine, which also inhibited c-Jun phosphorylation. Moreover, Q-VD-OPH, SP600125, and roscovitine partially reduced EHDV2-IBA-induced cell death, and roscovitine diminished the induction of autophagy by EHDV2-IBA. Taken together, our results imply that EHDV induces and benefits from the activation of signaling pathways involved in cell stress and death.

Published

2013

114. Dicodon monitoring of protein synthesis (DiCoMPS) reveals levels of synthesis of a viral protein in single cells.

Author

Barhoom S, Farrell I, Shai B, Dahary D, Cooperman BS, Smilansky Z, Elroy-Stein O, and Ehrlich M

Subjects

Animals, CHO Cells, Cells, Cultured, Codon, Cricetinae, Cricetulus, Hemorrhagic Disease Virus, Epizootic, RNA Interference, RNA, Transfer chemistry, RNA, Transfer metabolism, Single-Cell Analysis, Viral Nonstructural Proteins biosynthesis, Viral Nonstructural Proteins genetics, Fluorescence Resonance Energy Transfer methods, Protein Biosynthesis, Viral Proteins biosynthesis

Abstract

The current report represents a further advancement of our previously reported technology termed Fluorescent transfer RNA (tRNA) for Translation Monitoring (FtTM), for monitoring of active global protein synthesis sites in single live cells. FtTM measures Förster resonance energy transfer (FRET) signals, generated when fluorescent tRNAs (fl-tRNAs), separately labeled as a FRET pair, occupy adjacent sites on the ribosome. The current technology, termed DiCodon Monitoring of Protein Synthesis (DiCoMPS), was developed for monitoring active synthesis of a specific protein. In DiCoMPS, specific fl-tRNA pair combinations are selected for transfection, based on the degree of enrichment of a dicodon sequence to which they bind in the mRNA of interest, relative to the background transcriptome of the cell in which the assay is performed. In this study, we used cells infected with the Epizootic Hemorrhagic Disease Virus 2-Ibaraki and measured, through DiCoMPS, the synthesis of the viral non-structural protein 3 (NS3), which is enriched in the AUA:AUA dicodon. fl-tRNA(Ile)UAU-generated FRET signals were specifically enhanced in infected cells, increased in the course of infection and were diminished on siRNA-mediated knockdown of NS3. Our results establish an experimental approach for the single-cell measurement of the levels of synthesis of a specific viral protein.

Published

2013

115. On defining quantifying and measuring the SNARC effect.

Author

Tzelgov J, Zohar-Shai B, and Nuerk HC

Published

2013

116. Neuregulin promotes incomplete autophagy of prostate cancer cells that is independent of mTOR pathway inhibition.

Author

Schmukler E, Shai B, Ehrlich M, and Pinkas-Kramarski R

Subjects

Acetylcysteine pharmacology, Adenine analogs & derivatives, Adenine pharmacology, Anthracenes pharmacology, Apoptosis Regulatory Proteins antagonists & inhibitors, Apoptosis Regulatory Proteins genetics, Apoptosis Regulatory Proteins metabolism, Autophagy drug effects, Autophagy physiology, Beclin-1, Cell Death drug effects, Cell Death physiology, Cell Line, Tumor, Humans, MAP Kinase Signaling System drug effects, Male, Membrane Proteins antagonists & inhibitors, Membrane Proteins genetics, Membrane Proteins metabolism, Neoplasms, Hormone-Dependent drug therapy, Neoplasms, Hormone-Dependent pathology, Neoplasms, Hormone-Dependent physiopathology, Neuregulins pharmacology, Prostatic Neoplasms drug therapy, Proto-Oncogene Proteins c-akt metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism, Reactive Oxygen Species metabolism, Recombinant Proteins pharmacology, Signal Transduction drug effects, TOR Serine-Threonine Kinases physiology, Neuregulins physiology, Prostatic Neoplasms pathology, Prostatic Neoplasms physiopathology, TOR Serine-Threonine Kinases antagonists & inhibitors

Abstract

Background: Growth factors activating the ErbB receptors have been described in prostate tumors. The androgen dependent prostate cancer cell line, LNCaP, expresses the ErbB-1, ErbB-2 and ErbB-3 receptor tyrosine kinases. Previously, it was demonstrated that NRG activates ErbB-2/ErbB-3 heterodimers to induce LNCaP cell death, whereas, EGF activates ErbB-1/ErbB-1 or ErbB-1/ErbB-2 dimers to induce cell growth and survival. It was also demonstrated that PI3K inhibitors repressed this cell death suggesting that in androgen deprived LNCaP cells, NRG activates a PI3K-dependent pathway associated with cell death., Methodology/principal Findings: In the present study we demonstrate that NRG induces autophagy in LNCaP cells, using LC3 as a marker. However, the autophagy induced by NRG may be incomplete since p62 levels elevate. We also demonstrated that NRG- induced autophagy is independent of mammalian target of rapamycin (mTOR) inhibition since NRG induces Akt and S6K activation. Interestingly, inhibition of reactive oxygen species (ROS) by N-acetylcysteine (NAC), inhibited NRG-induced autophagy and cell death. Our study also identified JNK and Beclin 1 as important components in NRG-induced autophagy and cell death. NRG induced elevation in JNK phosphorylation that was inhibited by NAC. Moreover, inhibitor of JNK inhibited NRG-induced autophagy and cell death. Also, in cells overexpressing Bcl-2 or cells expressing sh-RNA against Beclin 1, the effects of NRG, namely induction of autophagy and cell death, were inhibited., Conclusions/significance: Thus, in LNCaP cells, NRG-induces incomplete autophagy and cell death that depend on ROS levels. These effects of NRG are mediated by signaling pathway that activates JNK and Beclin 1, but is independent of mTOR inhibition.

Published

2012