Gemma Roest1, Evelien Hesemans2, Kirsten Welkenhuyzen3, Tomas Luyten4, Nikolai Engedal5, Geert Bultynck6, Jan B Parys7. 1. Laboratory for Molecular and Cellular Signaling, Department of Cellular and Molecular Medicine & Leuven Kanker Instituut, KU Leuven, Campus Gasthuisberg O/N-1 B-802, Herestraat 49, BE-3000 Leuven, Belgium. gemma.roest@kuleuven.be. 2. Laboratory for Molecular and Cellular Signaling, Department of Cellular and Molecular Medicine & Leuven Kanker Instituut, KU Leuven, Campus Gasthuisberg O/N-1 B-802, Herestraat 49, BE-3000 Leuven, Belgium. hesemans.evelien@kuleuven.be. 3. Laboratory for Molecular and Cellular Signaling, Department of Cellular and Molecular Medicine & Leuven Kanker Instituut, KU Leuven, Campus Gasthuisberg O/N-1 B-802, Herestraat 49, BE-3000 Leuven, Belgium. kirsten.welkenhuyzen@kuleuven.be. 4. Laboratory for Molecular and Cellular Signaling, Department of Cellular and Molecular Medicine & Leuven Kanker Instituut, KU Leuven, Campus Gasthuisberg O/N-1 B-802, Herestraat 49, BE-3000 Leuven, Belgium. tomas.luyten@kuleuven.be. 5. Centre for Molecular Medicine Norway, Nordic EMBL Partnership for Molecular Medicine, University of Oslo, P.O. Box 1137 Blindern, N-0318 Oslo, Norway. nikolai.engedal@ncmm.uio.no. 6. Laboratory for Molecular and Cellular Signaling, Department of Cellular and Molecular Medicine & Leuven Kanker Instituut, KU Leuven, Campus Gasthuisberg O/N-1 B-802, Herestraat 49, BE-3000 Leuven, Belgium. geert.bultynck@kuleuven.be. 7. Laboratory for Molecular and Cellular Signaling, Department of Cellular and Molecular Medicine & Leuven Kanker Instituut, KU Leuven, Campus Gasthuisberg O/N-1 B-802, Herestraat 49, BE-3000 Leuven, Belgium. jan.parys@kuleuven.be.
Abstract
Accumulation of misfolded proteins in the endoplasmic reticulum (ER) activates the unfolded protein response (UPR) to reduce protein load and restore homeostasis, including via induction of autophagy. We used the proline analogue l-azetidine-2-carboxylic acid (AZC) to induce ER stress, and assessed its effect on autophagy and Ca2+ homeostasis. Treatment with 5 mM AZC did not induce poly adenosine diphosphate ribose polymerase (PARP) cleavage while levels of binding immunoglobulin protein (BiP) and phosphorylated eukaryotic translation initiation factor 2α (eIF2α) increased and those of activating transcription factor 6 (ATF6) decreased, indicating activation of the protein kinase RNA-like ER kinase (PERK) and the ATF6 arms of the UPR but not of apoptosis. AZC treatment in combination with bafilomycin A1 (Baf A1) led to elevated levels of the lipidated form of the autophagy marker microtubule-associated protein light chain 3 (LC3), pointing to activation of autophagy. Using the specific PERK inhibitor AMG PERK 44, we could deduce that activation of the PERK branch is required for the AZC-induced lipidation of LC3. Moreover, both the levels of phospho-eIF2α and of lipidated LC3 were strongly reduced when cells were co-treated with the intracellular Ca2+ chelator 1,2-bis(O-aminophenoxy)ethane-N,N,N',N'-tetraaceticacid tetra(acetoxy-methyl) ester (BAPTA-AM) but not when co-treated with the Na⁺/K⁺ ATPase inhibitor ouabain, suggesting an essential role of Ca2+ in AZC-induced activation of the PERK arm of the UPR and LC3 lipidation. Finally, AZC did not trigger Ca2+ release from the ER though appeared to decrease the cytosolic Ca2+ rise induced by thapsigargin while also decreasing the time constant for Ca2+ clearance. The ER Ca2+ store content and mitochondrial Ca2+ uptake however remained unaffected.
Accumulation of misfolded proteins in the endoplasmic reticulum (ER) activates the unfolded protein response (UPR) to reduce protein load and restore homeostasis, including via induction of autophagy. We used the proline analogue l-azetidine-2-carboxylic acid (AZC) to induce ER stress, and assessed its effect on autophagy and Ca2+ homeostasis. Treatment with 5 mM AZC did not induce poly adenosine diphosphate ribose polymerase (PARP) cleavage while levels of binding immunoglobulin protein (BiP) and phosphorylated eukaryotic translation initiation factor 2α (eIF2α) increased and those of activating transcription factor 6 (ATF6) decreased, indicating activation of the protein kinase RNA-like ER kinase (PERK) and the ATF6 arms of the UPR but not of apoptosis. AZC treatment in combination with bafilomycin A1 (Baf A1) led to elevated levels of the lipidated form of the autophagy marker microtubule-associated protein light chain 3 (LC3), pointing to activation of autophagy. Using the specific PERK inhibitor AMG PERK 44, we could deduce that activation of the PERK branch is required for the AZC-induced lipidation of LC3. Moreover, both the levels of phospho-eIF2α and of lipidated LC3 were strongly reduced when cells were co-treated with the intracellular Ca2+ chelator 1,2-bis(O-aminophenoxy)ethane-N,N,N',N'-tetraaceticacid tetra(acetoxy-methyl) ester (BAPTA-AM) but not when co-treated with the Na⁺/K⁺ ATPase inhibitor ouabain, suggesting an essential role of Ca2+ in AZC-induced activation of the PERK arm of the UPR and LC3 lipidation. Finally, AZC did not trigger Ca2+ release from the ER though appeared to decrease the cytosolic Ca2+ rise induced by thapsigargin while also decreasing the time constant for Ca2+ clearance. The ER Ca2+ store content and mitochondrial Ca2+ uptake however remained unaffected.
Entities:
Keywords:
Ca2+; ER stress; PERK; UPR; autophagy; l-azetidine-2-carboxylic acid
Endoplasmic reticulum (ER) stress is a particular form of cellular stress that occurs when the ER machinery is overwhelmed by the amount of unfolded or misfolded proteins [1]. To restore ER homeostasis, a complex program is engaged that is called the unfolded protein response (UPR), and which consists of three arms, each depending on the activation of a distinct ER stress sensor, i.e., inositol-requiring enzyme 1 (IRE1), activating transcription factor (ATF) 6, and protein kinase RNA-like ER kinase (PERK). PERK activation leads to eukaryotic translation initiator factor 2α (eIF2α) phosphorylation and reduction of general protein translation, while IRE1 activation initiates mRNA degradation. Additionally, translocation of proteins into the ER is inhibited and macroautophagy (further called autophagy) is induced to eliminate damaged ER and to remove abnormal protein aggregates [2]. Furthermore, transcription factors dependent on each of the three arms of the response trigger the expression of a large variety of genes encoding proteins associated with ER-associated degradation, ER protein import, protein folding, lipid synthesis (needed for ER membrane expansion), as well as pro-survival genes including genes related to autophagy. The latter process largely depends on the PERK arm of the UPR that via eIF2α phosphorylation leads to the selective translation of ATF4 [2]. If the ER stress condition cannot be resolved, cell demise by apoptosis is eventually triggered [3].Autophagy is an important, evolutionary conserved pro-survival process that promotes cellular homeostasis. Long-lived proteins and dysfunctional organelles are thereby engulfed in newly formed double-membrane vesicles called autophagosomes, which eventually will undergo fusion with lysosomes. In the resulting autolysosomes, the autophagosomes and their cargo are degraded and the components recycled [4].A basal level of autophagy is always needed for the cell, but when cells undergo stress the autophagy pathway is upregulated in order to cope with the new situation and to regain cellular homeostasis. Apart from ER stress, cellular stress can also be the consequence of e.g., starvation conditions, the presence of intracellular pathogens or pharmacological compounds that induce autophagy [5]. It is a highly regulated process, which can be activated by adenosine monophosphate (AMP)-activated protein kinase or inhibited by the mechanistic target of rapamycin (mTOR) and that is further regulated by over 30 autophagy-related (ATG) proteins [6]. A long-standing question concerns the role of intracellular Ca2+ signaling in the regulation of the autophagic process and especially whether the role is stimulatory or inhibitory as evidence for both mechanisms have been proposed (recently reviewed in [7]).ER stress itself is intimately linked to intracellular Ca2+ handling [8,9,10,11,12,13,14]. Treatment of cells with thapsigargin (TG) or cyclopiazonic acid, inhibitors of the sarco/endoplasmic Ca2+ ATPase (SERCA), leads to ER Ca2+ depletion and ER stress [15,16,17,18]. This is due to the fact that many ER chaperones play a dual role by not only participating in protein folding and maturation but also by binding the Ca2+ ions in the lumen of the ER [14].Previous work by our own group had shown that intracellular Ca2+ was required for autophagic flux induced by either nutrient starvation [19], rapamycin treatment [20], or resveratrol treatment [21]. This conclusion was supported by the fact that incubation with the intracellular Ca2+ chelator 1,2-bis(O-aminophenoxy)ethane-N,N,N′,N′-tetraacetic acid tetra(acetoxymethyl) ester (BAPTA-AM), the inositol 1,4,5-trisphosphate receptor (IP3R) inhibitor Xestospongin B and/or IP3R knockout all inhibited autophagy induction. Moreover, these results are fully in line with those obtained by other groups [22,23,24,25,26,27,28]. However, at the best of our knowledge the Ca2+ sensitivity of autophagy occurring after ER stress as part of the UPR has never been tested, and it was the aim of this study to investigate this point.As for obvious reasons it was not appropriate to induce ER stress via a mechanism that by itself modified intracellular Ca2+, we could not use TG. Moreover, since autophagy and apoptosis influence each other [29,30,31] and apoptosis can occur subsequently to Ca2+ release by the IP3R and mitochondrial Ca2+ overload [32,33,34,35,36], we also had to avoid ER stress inducers that led to rapid apoptosis of the cells. We therefore focused on l-azetidine-2-carboxylic acid (AZC), a proline analog (Figure 1A) known to induce protein misfolding and aggregation and subsequent ER stress [37,38,39,40,41].
Figure 1
(A) l-azetidine-2-carboxylic acid (AZC) is an analog of proline. (B) AZC induces cleavage of ATF6 and upregulates BiP expression and phospho-eIF2α levels, but does not affect ERp57 or ERp72 expression. Cells were treated for 6 h with DMSO or 1 μM staurosporine (STS) as control, or for 0–9 h with 5 mM AZC, and during the last 4 h 100 nM Baf A1 was added. A representative blot for six independent experiments each performed in duplicate showing protein levels of ER stress markers ATF6, BiP, ERp72, ERp57, total eIF2α, and phospho-eIF2α. Vinculin was used as loading control. (C) Quantification of ER stress markers in B shown as mean ± SEM relative to 0 h AZC. * p < 0.05, ** p < 0.01, *** p < 0.001. (D) Representative RT-PCR gel of unspliced and spliced XBP1 mRNA levels of three independent experiments each performed in duplicate.
Our results indicate that Ca2+ plays an important role in the development of both the UPR and autophagy upon AZC treatment.
2. Materials and Methods
2.1. Cell Culture
HeLa cells were cultured at 37 °C and 5% CO2 in Dulbecco’s Modified Eagle Medium supplemented with 10% heat-inactivated fetal bovine serum (FBS), GlutaMAX (Gibco/Invitrogen, Merelbeke, Belgium; # 35050) and penicillin and streptomycin (Gibco/Invitrogen; # 15070-063), as described before [19,20,21]. Cells were washed with phosphate-buffered saline (PBS) and supplied with fresh medium two hours before the start of each experiment. The cell line has been authenticated using autosomal Short Tandem Repeat profiling performed by the University of Arizona Genetics Core and fully matched the DNA fingerprint present in the reference database.
2.3. Sodium Dodecyl Sulfate (SDS) Polyacrylamide Gel Electrophoresis and Western Blotting
Cells were washed with PBS and lysed with lysis buffer (150 mM Hepes (pH 7.5), 150 mM NaCl, 100 mM NaF, 10 mM ethylene diamine tetraacetic acid (EDTA), 10 mM Na4P2O7, 1% Triton-X-100, 0.1% SDS, EDTA-free protease inhibitor (Thermo Fisher Scientific; # 88266), PhosSTOP phosphatase inhibitor (Sigma-Aldrich; # 04906837001)). Lysates were incubated on ice for 30 min and centrifuged for 5 min at 8000× g. Protein concentration of the supernatant was determined using a bicinchonic acid protein assay kit and bovine serum albumin standards (Thermo Fisher Scientific; # 23225). Proteins were then separated on 10–20% Tris-glycine gels (Thermo Fisher Scientific) using Tris-glycine running buffer (Thermo Fisher Scientific; # LC2675). Proteins were transferred to polyvinylidene difluoride membrane in running buffer (25 mM Trizma base, 192 mM glycine) containing 10% methanol and blocked in 5% non-fat milk in Tris-buffered saline (TBS) containing 0.1% Tween. Membranes were incubated with primary antibodies overnight at 4 °C, and horseradish peroxidase-conjugated secondary antibodies for 1 h at room temperature. Proteins were detected using Clarity Western Enhanced Chemiluminescence (ECL) Substrate (Biorad, Temse, Belgium; # 170-5061) or ECL Western Blotting Substrate (Thermo Fisher Scientific; 32106). Individual experiments were always performed in duplicate.
2.4. XBP1 Splicing
Cells were trypsinized and centrifuged for 5 min at 500× g. RNA was extracted using the High Pure RNA Isolation kit (Roche, Mannheim, Germany; # 11828665001) according to manufacturer’s protocol. cDNA was prepared using the High Capacity cDNA Reverse Transcription kit (Applied Biosystems, Brussels, Belgium; # 4368814) according to manufacturer’s protocol. XBP1 mRNA was amplified using GoTaq Green master mix (Promega, Leiden, The Netherlands; # M7112) and XBP1 specific primers (IDT, Leuven, Belgium) and separated on a 2.5% Ultrapure agarose (Invitrogen, # 16500-500) gel containing 0.005% EtBr (Invitrogen, # 15585-011). Individual experiments were always performed in duplicate.
2.5. Cell Death Assays
Cell death was assessed by PARP cleavage and by propidium iodide (PI) staining. PARP cleavage was assessed by Western blotting as described in Section 2.3. PI staining was performed essentially as previously described [43]. Briefly, cells were plated in 96-well plates and stained with 2.5 μg/mL PI (Thermo Fisher Scientific; # P3566). Cells were treated with 0–25 mM AZC, and the PI fluorescence was monitored for a total of 72 h in an IncuCyte Zoom (Essen Bioscience, Welwyn Garden City, UK) with a 4 h interval between scans. Individual experiments were always performed in triplicate.
2.6. Ca2+ Measurements at the Population Level
Cells were plated in 96-well plates and treated as indicated. During the last hour of treatment the cells were loaded for 30 min with 1.8 μM Fura-2 AM followed by 30 min de-esterification in modified Krebs solution (150 mM NaCl, 5.9 mM KCl, 1.2 mM MgCl2, 11.6 mM Hepes (pH 7.3), 11.5 mM glucose, 1.5 mM CaCl2). Fluorescence was measured on a FlexStation 3 microplate reader (Molecular Devices, Sunnyvale, CA, USA) by alternate excitation at 340 nm and 380 nm and recording emission at 510 nm. Compounds were added as indicated. Individual experiments were always performed in triplicate.
2.7. Single-Cell Ca2+ Measurements
ER and mitochondrial Ca2+ levels were measured with the genetically encoded Ca2+ indicators G-CEPIA1er and R-GECO1mt [44] kindly provided by Dr. M. Iino (The University of Tokyo, Tokyo, Japan). Cells were transfected with 300 ng G-CEPIA1er and 600 ng R-GECO1mt using X-treme Gene HP DNA (Roche; # 06366546001) according to the manufacturer’s protocol. After 48 h single-cell measurements were performed on a Zeiss Axio Observer Z1 Inverted Microscope equipped with a 20× air objective and a high-speed digital camera (Axiocam Hsm, Zeiss, Jena, Germany). Extracellular Ca2+ was chelated with 3 mM ethylene glycol tetraacetic acid (EGTA) and one minute later the indicated compound was added. Changes in G-CEPIA1er fluorescence were followed after excitation at 480 nm and measurement of emission at 520 nm. Changes in R-GECO1mt fluorescence were followed after excitation at 377 nm and measurement of emission at 466 nm. The traces were normalized to baseline fluorescence (F/F0) where the baseline was calculated as the average of the first six time points. At least 99 cells per condition were measured in the course of six individual experiments.
2.8. Statistics
Results are presented as mean ± standard error of the mean (SEM). Significance was tested using a one-way analysis of variance with Tukey post-hoc test. Results were considered significant when p < 0.05.
3. Results
3.1. AZC Upregulates the Levels of BiP and Phospho-eIF2α while Decreasing the Level of Full-Length ATF6
To analyze the induction of ER stress, HeLa cells were treated with 5 mM AZC for up to 9 h. The cell lysates were analyzed by Western blotting for the ER stress markers ATF6, binding immunoglobulin protein (BiP), ER protein (ERp) 72, ERp57, and total and phospho-eIF2α (Figure 1B,C). AZC treatment led to a 2.5-fold decrease in full-length ATF6 (already significantly decreased after 3 h), a 1.5-fold increase of BiP protein levels (already significantly increased after 6 h), and a 2-fold increase in the levels of phospho-eIF2α (already significantly increased after 3 h). The total level of eIF2α only decreased after treatment with AZC for 9 h, while ERp57 or ERp72 protein levels did not change in response to AZC treatment. To evaluate the activation of the IRE1α arm of the UPR, we performed an X-box protein (XBP) 1 splicing assay. AZC treatment did not significantly induce XBP1 splicing (Figure 1D). Staurosporine (STS, 1 µM) was used as a positive control for activation of ER stress [45] and cell death [46,47,48]. STS treatment for 6 h resulted in a 10-fold reduction in the level of full-length ATF6, a two-fold downregulation of ERp57 protein levels, an approximately nine-fold increase in the levels of phospho-eIF2α and a substantial production of spliced XBP1, but did not modify BiP levels.Taken together, these results indicate that a 6 h treatment with AZC activates both the PERK and the ATF6 arm of the UPR, resulting in upregulated BiP protein expression and increased phosphorylation of eIF2α.
3.2. AZC Does Not Induce Cell Death within 6 h of Treatment
Because it was important to study ER stress and subsequent autophagy in conditions where cell death was not induced, we assessed the levels of cleaved poly adenosine diphosphate ribose polymerase (PARP) upon AZC treatment during the same time period. While STS led to clear PARP cleavage, we observed virtually no cleavage upon AZC treatment (Figure 2A). The quantification of these results is shown in Figure 2B. Additionally, we evaluated the cellular toxicity of various AZC concentrations as a function of time by monitoring the increase of PI-positive cells. These results indicated a dose-dependent increase of PI-positive cells with time starting only after at least 12 h of treatment with AZC, even at high AZC concentrations (10–25 mM). Moreover, even after 72 h, 5 mM AZC induced less than 10% cell death above the vehicle control condition.
Figure 2
AZC does not induce cell death within 6 h of treatment. (A) A representative blot of six independent experiments each performed in duplicates showing protein levels of uncleaved and cleaved poly adenosine diphosphate ribose polymerase (PARP). Cells were treated for 6 h with DMSO or 1 μM staurosporine (STS) as control, or for 0–9 h with 5 mM AZC, and during the last 4 h 100 nM Baf A1 was added. Vinculin was used as loading control. (B) Quantification of PARP cleavage in (A) shown as mean ± SEM relative to 0 h AZC. (C) AZC induces cell death in a concentration-dependent manner only from 12 h of treatment. Cells were stained with 2.5 μg/mL propidium iodide (PI) and treated with 0–25 mM AZC for 72 h. Results are shown as average ± SEM (indicated by the dotted lines) of two experiments each performed in triplicate.
From both the PARP-cleavage analysis and the PI staining, we can conclude that treatment with 5 mM AZC for 6 h did not lead to any significant cell death.
3.3. AZC Increases the Levels of Lipidated Autophagy Marker LC3
To avoid interference of ER stress-induced cell death, we wanted to use conditions that allowed induction of the UPR and of autophagy in a time frame as short as possible. Based on the results presented in Figure 1 (activation of the UPR) and in Figure 2 (absence of cell death), we decided to select a 6 h incubation time with 5 mM AZC to assess the levels of the autophagy marker lipidated microtubule-associated protein light chain 3 (LC3-II). In order to evaluate autophagy induction upon AZC treatment, autolysosomal degradation was inhibited by addition of 100 nM bafilomycin A1 (Baf A1) during the last 4 h of AZC treatment. In the absence of Baf A1, AZC increased the levels of LC3-II 3-fold as assessed by Western blotting (Figure 3A). Co-treatment with Baf A1 increased the levels of LC3-II about 8- and 13-fold in control and AZC-treated cells, respectively. Figure 3B shows the quantification from twelve independent experiments.
Figure 3
AZC induces autophagy. Cells were treated for 6 h with 5 mM AZC, and during the last 4 h 100 nM bafilomycin A1 (Baf A1) was added to inhibit autolysosomal degradation. (A) A representative blot of twelve independent experiments each performed in duplicate showing LC3-II protein levels. Glyceraldehyde 3-phosphate dehydrogenase (GAPDH) was used as loading control. (B) Quantification of LC3-II levels in (A) shown as mean ± SEM relative to untreated control. ** p < 0.01, *** p < 0.001.
The larger increase of LC3-II levels in AZC-treated cells in the presence of Baf A1 as compared to the control conditions suggests that the upregulation of LC3-II levels does not depend on a block of autophagosome-lysosome fusion and/or of lysosomal degradative activity but is related to the induction of autophagy.
3.4. AZC Upregulates the Levels of LC3-II Subsequently to Activation of the PERK Pathway
To investigate the relation between the UPR and the increased LC3-II levels after application of AZC, we used the PERK-selective inhibitor AMG PERK 44 [49]. AMG PERK 44 (1–5 µM) did neither affect ATF6 cleavage nor BiP induction (Figure 4A,B). Not only the AZC-induced increase in phospho-eIF2α was abolished, as was anticipated, but also the AZC-induced increase in LC3-II in spite of the fact that the ATF6 pathway remained active.
Figure 4
AZC elevates LC3-II levels in a PERK-dependent manner. Cells were treated for 6 h with 5 mM AZC in absence or presence of 1 μM, 2.5 μM, or 5 μM of the PERK inhibitor AMG PERK 44, and during the last 4 h 100 nM Baf A1 was added. (A) A representative blot for six independent experiments each performed in duplicate in absence or presence of AMG PERK 44 (2.5 and 5 μM) showing protein levels of ER stress markers ATF6, BiP, total eIF2α, and phospho-eIF2α and of autophagy marker LC3-II. Vinculin was used as loading control. (B) Quantification of ER stress and autophagy markers in (A) as well as of independent experiments performed in absence or presence of AMG PERK 44 (1–5 μM), shown as mean ± SEM relative to untreated control. * p < 0.05, ** p < 0.01, *** p < 0.001.
These results indicate that activation of the PERK pathway is a prerequisite for the occurrence of the AZC-induced increase in LC3-II levels, and that the ATF6 branch of the UPR is not sufficient for obtaining this effect.
3.5. AZC Upregulates the Levels of LC3-II in a Ca2+-Dependent Manner
To investigate the role of Ca2+ in the elevation of LC3-II levels triggered by AZC, we co-treated the cells with increasing concentrations of the intracellular Ca2+ chelator BAPTA-AM. This led to a dose-dependent reduction of the AZC-induced increase in LC3-II (Figure 5A). Figure 5B shows the quantification from six individual experiments.
Figure 5
AZC elevates LC3-II levels in a Ca2+-dependent manner. Cells were treated for 6 h with 5 mM AZC in absence or presence of 10 μM or 20 μM of the intracellular Ca2+ chelator BAPTA-AM, and during the last 4 h 100 nM Baf A1 was added. (A) A representative blot of six independent experiments each performed in duplicate, assessing protein levels of the autophagy marker LC3-II. Glyceraldehyde 3-phosphate dehydrogenase (GAPDH) was used as loading control. (B) Quantification of LC3-II levels in (A) shown as mean ± SEM relative to untreated control. * p < 0.05.
These results strongly suggest that the AZC-induced increase in LC3-II requires intracellular Ca2+.
3.6. AZC-Induced Elevation of Phospho-eIF2α Levels Is Ca2+ Dependent
The link between ER stress induction and autophagy involves several steps. In order to identify which steps are sensitive to Ca2+, we assessed the effect of BAPTA-AM on the AZC-induced upregulation of BiP expression levels, and on the levels of phospho-eIF2α. While there was no effect of BAPTA-AM treatment on BiP levels, we observed a significant reduction of AZC-induced elevation of phospho-eIF2α upon co-treatment with BAPTA-AM (Figure 6A,B). Additionally, we verified that BAPTA-AM treatment did not result in PARP cleavage (Figure 6A).
Figure 6
AZC-induced elevation of phospho-eIF2α levels is Ca2+ dependent. Cells were treated for 6 h with 5 mM AZC in absence or presence of 10 μM or 20 μM of the intracellular Ca2+ chelator BAPTA-AM and during the last 4 h 100 nM Baf A1 was added. (A) Representative blot of six independent experiments each performed in duplicate showing protein levels of the cell death marker PARP, and of ER stress markers BiP, total eIF2α and phospho-eIF2α. Vinculin was used as loading control. (B) Quantification of ER stress markers in (A) shown as mean ± SEM relative to untreated control. ** p < 0.01, *** p < 0.001.
These results indicate that levels of phospho-eIF2α induced by AZC is dependent on Ca2+, and may thus constitute an upstream event to the sensitivity of the subsequent autophagic process to Ca2+.
3.7. Effects of BAPTA-AM Treatment Are Not Related to Na+/K+ ATPase Inhibition
Recently, it was shown that BAPTA-AM can also affect Na+/K+ ATPase activity [50]. To discriminate the Ca2+-chelating role of BAPTA-AM from its inhibitory effect on the Na+/K+ ATPase, we combined AZC treatment with various concentrations of the specific Na+/K+ ATPase inhibitor ouabain and assessed the levels of total and phospho-eIF2α and the levels of LC3-II. In contrast to the effects observed with BAPTA-AM, increasing ouabain concentrations resulted in strongly increased levels of phospho-eIF2α, while LC3-II levels generally increased up to 500 nM ouabain followed by a decrease at the highest used concentration of ouabain (Figure 7A,B). Moreover, these effects occurred independently of the absence or presence of AZC.
Figure 7
Ouabain affects ER stress, apoptosis and autophagy markers differently than BAPTA-AM. Cells were treated for 6 h with 5 mM AZC in absence or presence of 10 nM, 500 nM, or 1 μM of the Na+/K+ ATPase inhibitor ouabain, and during the last 4 h 100 nM Baf A1 was added. (A) A representative blot of eight independent experiments each performed in duplicate showing levels of total eIF2α and phospho-eIF2α, and of LC3-II. Vinculin was used as loading control. (B) Quantification of protein levels in (A) shown as mean ± SEM relative to untreated control. * p < 0.05, ** p < 0.01.
These results are therefore distinct from those obtained with BAPTA-AM (Figure 5 and Figure 6) and thus support a role for intracellular Ca2+ in AZC-induced ER stress and autophagy.
3.8. Pretreatment with AZC Reduces the Cytosolic Amount of Ca2+ after ER Store Release
To determine the relation between AZC treatment and intracellular Ca2+ handling, we investigated whether AZC treatment directly impacts the Ca2+ stores. We therefore loaded the cells with the cytosolic Ca2+ indicator Fura-2 AM and followed its fluorescence on a FlexStation 3 microplate reader. To prevent influx of Ca2+ in the cell, the extracellular Ca2+ was first chelated by addition of 3 mM EGTA, and the SERCA inhibitor TG was subsequently used to uncover Ca2+ release from the ER. While TG led to an increase in cytosolic [Ca2+], acute application of either 5 mM or 10 mM AZC did not provoke a rise in cytosolic [Ca2+] (Figure 8A). However, when cells were pre-treated for 6 h with 5 mM or 10 mM AZC and TG-induced [Ca2+] elevations were monitored, we noticed a lower rise of cytosolic Ca2+ in the pre-treated samples as compared to the control samples (Figure 8B). This was reflected by a ~35% lower area under the curve (Figure 8C). Additionally, the clearance of Ca2+ from the cytosol appeared faster after AZC pretreatment, as indicated by a ~42% lower τ value for the decline phase of the Fura-2 AM signal (Figure 8D).
Figure 8
AZC does not acutely affect cytosolic Ca2+ but pretreatment with AZC reduces the Ca2+ amount detected in the cytosol after ER Ca2+ store release evoked by thapsigargin (TG). Results are shown as mean ± SEM (indicated by the dotted lines) of three independent experiments each performed in duplicate. (A) Cells were loaded with 1.8 μM Fura-2 AM for 30 min, followed by 30 min of deesterification. Fura-2 AM fluorescence was monitored using a FlexStation 3 microplate reader. Extracellular Ca2+ was chelated with 3 mM EGTA and 120 s later AZC or 1 μM TG (as a positive control) was added as indicated. (B) Cells were pretreated for 6 h with 5 mM or 10 mM AZC. During the last hour of treatment, cells were loaded with 1.8 μM Fura-2 AM for 30 min, followed by 30 min of deesterification. Extracellular Ca2+ was chelated with 3 mM EGTA and 120 s later 1 μM TG or Krebs solution (vehicle) was added as indicated. (C) Quantification of the area under the curve of the Ca2+ traces in (B) * p < 0.05. (D) Time constant τ for the decline phase of the Ca2+ traces in (B) *** p < 0.001.
In short, AZC does not have an acute effect on intracellular Ca2+, though a prolonged incubation with the compound appears to modulate intracellular Ca2+ signaling in a complex way.
3.9. AZC Does Not Affect the ER Ca2+ Store Content or the ER-Mitochondrial Ca2+ Transfer
Because we observed a lower rise in cytosolic [Ca2+] upon application of TG after pretreatment with AZC, we hypothesized that AZC may lower the ER Ca2+ store content, or that Ca2+ transfer to the mitochondria may have been increased. In order to investigate this, we co-transfected cells with both G-CEPIA1er and R-GECO1mt to simultaneously detect ER Ca2+ and mitochondrial Ca2+, and treated the cells for 6 h with 5 mM or 10 mM AZC. EGTA was then applied and Ca2+ released from the ER with TG. Surprisingly, we did not detect differences in the ER Ca2+-leak rates between cells pretreated with either 5 mM or 10 mM AZC and untreated control cells (Figure 9A). Furthermore, the amount of Ca2+ transferred into the mitochondria after TG application was also very similar between AZC-treated cells and untreated cells (Figure 9B). Finally, the difference in the TG-triggered cytosolic [Ca2+] rise between AZC-treated and untreated cells could also not be linked to a change in expression levels of any of the major Ca2+-transport proteins, such as IP3Rs, PMCAs, SERCA2B, or the mitochondrial Ca2+ uniporter (MCU) (Figure 9C,D).
Figure 9
AZC does not affect the ER store content or ER-mitochondrial Ca2+ transfer. Cells were transfected with the Ca2+ sensors G-CEPIA1er and R-GECO1mt. At 48 h after transfection, cells were pretreated with 5 mM or 10 mM AZC for 6 h. Extracellular Ca2+ was chelated with 3 mM EGTA and 60 s later ER Ca2+ release was uncovered with 1 μM thapsigargin (TG) as indicated. At least 99 cells in six independent experiments were measured and results are shown as mean ± SEM (indicated by the dotted lines). (A) AZC pretreatment did not change the properties of the ER Ca2+ store as detected by G-CEPIA1er. (B) AZC pretreatment did not affect uptake by the mitochondria of ER-released Ca2+ as detected by R-GECO1mt. The insert shows the quantification of the area under the curve of traces showing Ca2+ uptake by the mitochondria. (C) AZC treatment does not affect the expression levels of the IP3Rs, the plasma membrane Ca2+ ATPases (PMCA), SERCA2B or the mitochondrial Ca2+ uniporter (MCU). A representative blot of eight independent experiments each performed in duplicate is shown. Vinculin was used as loading control. (D) Quantification of protein levels in (C) shown as mean ± SEM relative to untreated control.
Taken together, long-term treatment of cells with AZC (6 h) seems to modify cellular Ca2+ handling, though without directly affecting the ER Ca2+ leak, ER-mitochondrial Ca2+ transfer or the expression of IP3Rs, PMCAs, SERCA2B, and the MCU.
4. Discussion
One of the main functions of the ER is the proper folding of nascent proteins. To ensure this, chaperones assist and correct the process when necessary [51]. Stress conditions including oxidative stress or high temperatures can disturb the folding and cause an accumulation of misfolded proteins in the ER and subsequently ER stress. Activation of the UPR can resolve this situation but failure to do so may result in accumulation of protein aggregates and eventually cell death [52]. Prolonged ER stress may also be involved in neurodegenerative diseases including Alzheimer’s disease, type 2 diabetes, and cancer [53].Classic chemical ER stress inducers include dithiothreitol, tunicamycin, and TG. In our preliminary experiments however, these compounds also showed induction of apoptosis or they displayed an intrinsic effect on Ca2+ homeostasis. Therefore, we turned to AZC. This proline analogue contains a four-membered carbon ring in contrast to the five-membered ring in proline (Figure 1A). Incorporation of AZC in proteins leads to an altered tertiary protein structure and accumulation of protein aggregates [37,38,54]. Our results indicate that this activates in HeLa cells the PERK and the ATF6 arms of the UPR but not the IRE1 arm (Figure 1). This is in line with the results of Qian et al. who in HEK293 cells found a dose- and time-dependent increase of phospho-eIF2α upon AZC treatment [39], and with Shang et al. who showed that significant XBP1 splicing requires very high concentrations of AZC [41]. The former correlated with a decrease in phosphorylation of ribosomal protein S6, indicating inhibition of the autophagy suppressor mTOR. This is in line with our results with Baf A1 (Figure 3), which suggest a role of AZC in the induction of autophagy. Moreover, using the specific PERK inhibitor AMG PERK 44, we can conclude that activation of the PERK arm of the UPR is absolutely needed for the subsequent increase in LC3-II levels by AZC. Finally, Nivon et al. showed that AZC treatment causes the formation of protein aggregates in HeLa cells and that this correlates with an NFκB-dependent increase in LC3-II levels [38].Ca2+ plays an important role in both ER stress and autophagy [7,9,14]. In autophagy, depending on the exact conditions both inhibitory and stimulatory effects of Ca2+ were described [7,55]. To assess the role of Ca2+ in intracellular processes like autophagy, treatment with the intracellular Ca2+ chelator BAPTA-AM is the favored technique [7]. We therefore co-treated our cells with AZC and BAPTA-AM, upon which we observed a decrease of AZC-induced elevation of phospho-eIF2α as well as of LC3-II (Figure 5 and Figure 6). However, recently it was shown that various related Ca2+-binding molecules, including BAPTA-AM, can inhibit the Na+/K+ ATPase, independently of their Ca2+-binding affinity [50]. Although in the latter study, BAPTA-AM was a less potent Na+/K+ ATPase inhibitor than the other compounds tested, it readily accumulates in the cell and we therefore wanted to verify whether Na+/K+ ATPase inhibition by BAPTA-AM could affect the interpretation of our results. One way to discriminate between the Ca2+ chelating and the Na+/K+ ATPase inhibiting effect of BAPTA-AM, is to assess whether the effects provoked by BAPTA-AM are replicated by the well-known specific Na+/K+ ATPase inhibitor ouabain [56]. All human Na+/K+ ATPase isozymes are characterized by a Kd for ouabain between 13 and 37 nM [57]. In order to encompass various levels of Na+/K+ ATPase inhibition, we applied a range of concentrations of ouabain between 10 nM and 1 µM. However, at none of these concentrations did ouabain (Figure 7) mimic the effect of BAPTA-AM on AZC-induced elevation of phosphorylated eIF2α and LC3-II (Figure 5 and Figure 6). Therefore, we conclude that these effects represent a bona fide contribution of Ca2+ chelation rather than Na+/K+ ATPase inhibition and that intracellular Ca2+ is critical for both AZC-induced ER stress and elevation of LC3-II.Interestingly, our data indicate an essential role of Ca2+ in AZC-induced elevation of phospho-eIF2α. Given that the PERK-arm of the UPR has been reported to be required for ER stress-mediated induction of LC3-II [58,59], this finding may form a link with the requirement for Ca2+ observed for the subsequent elevation of LC3-II levels. Whereas Ca2+ was recently shown to be required for non-UPR-related functions of PERK [60], our study indicates that Ca2+ is also required for efficient eIF2α phosphorylation, and thus for transduction of PERK-arm mediated UPR signaling. On the other hand, Ca2+ did not seem to be required for AZC-mediated upregulation of BiP. The Ca2+ sensitivities of the different parts of the UPR signal transduction pathways remain to be determined, but it is already noteworthy that the BiP upregulation is insensitive to both the PERK inhibitor and to BAPTA-AM.Finally, we found that 6 h of pre-treatment with 5–10 mM AZC reduced the amount of Ca2+ released from the ER Ca2+ store with TG, but did not induce Ca2+ release itself (Figure 8 and Figure 9A). These results are in agreement with those of Caspersen et al. who previously demonstrated in PC12 cells that AZC did not induce Ca2+ release from the ER by itself although they also claim that the ER is not significantly depleted after pre-treatment for 4 h with 5 mM AZC [61]. However, in the latter study, no quantification of the Ca2+ signal was performed, and on the traces shown the agonist-induced Ca2+ release is anyway smaller than in control conditions.We initially hypothesized that the reduction in TG-induced cytosolic Ca2+ rise after pre-incubation with AZC may be due to a reduced Ca2+ content in the ER and therefore a lower release of Ca2+ into the cytosol upon TG application, or due to an increased Ca2+ transfer from ER to mitochondria, thereby preventing detection of the Ca2+ in the cytosol. However, when measuring Ca2+ simultaneously in the ER and the mitochondria, we did neither observe a reduction in ER store content nor an increase in mitochondrial Ca2+ transfer in cells pretreated for 6 h with 5 or 10 mM AZC as compared to control cells (Figure 9A,B). We therefore speculate that pre-treatment with AZC affects Ca2+-transport systems outside the ER and mitochondrial compartments. For instance, it is possible that PMCA, responsible for exporting Ca2+ from the cytosol to the extracellular environment, is affected. We could exclude a modification in PMCA expression levels (Figure 9C) though a change in activity remains possible. A more efficient export of Ca2+ from the cytosol by PMCA may lead to an apparent reduction of the amount of cytosolic Ca2+ without an actual decrease of the ER Ca2+ store content, and thus explain the reduced τ value for the clearance of Ca2+ from the cytosol.Taken together, our results indicate a critical role for Ca2+ in the process of eIF2α phosphorylation and LC3-II production upon AZC treatment. AZC however does not directly affect ER Ca2+ store content or ER-to-mitochondria Ca2+ transfer and the observed effects on intracellular Ca2+ handling are likely not related to its effect on UPR and autophagy.
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Roberta A Gottlieb; Illana Gozes; Devrim Gozuacik; Martin Graef; Markus H Gräler; Veronica Granatiero; Daniel Grasso; Joshua P Gray; Douglas R Green; Alexander Greenhough; Stephen L Gregory; Edward F Griffin; Mark W Grinstaff; Frederic Gros; Charles Grose; Angelina S Gross; Florian Gruber; Paolo Grumati; Tilman Grune; Xueyan Gu; Jun-Lin Guan; Carlos M Guardia; Kishore Guda; Flora Guerra; Consuelo Guerri; Prasun Guha; Carlos Guillén; Shashi Gujar; Anna Gukovskaya; Ilya Gukovsky; Jan Gunst; Andreas Günther; Anyonya R Guntur; Chuanyong Guo; Chun Guo; Hongqing Guo; Lian-Wang Guo; Ming Guo; Pawan Gupta; Shashi Kumar Gupta; Swapnil Gupta; Veer Bala Gupta; Vivek Gupta; Asa B Gustafsson; David D Gutterman; Ranjitha H B; Annakaisa Haapasalo; James E Haber; Aleksandra Hać; Shinji Hadano; Anders J Hafrén; Mansour Haidar; Belinda S Hall; Gunnel Halldén; Anne Hamacher-Brady; Andrea Hamann; Maho Hamasaki; Weidong Han; Malene Hansen; Phyllis I Hanson; Zijian Hao; Masaru Harada; Ljubica Harhaji-Trajkovic; Nirmala Hariharan; Nigil Haroon; James Harris; Takafumi Hasegawa; Noor Hasima Nagoor; Jeffrey A Haspel; Volker Haucke; Wayne D Hawkins; Bruce A Hay; Cole M Haynes; Soren B Hayrabedyan; Thomas S Hays; Congcong He; Qin He; Rong-Rong He; You-Wen He; Yu-Ying He; Yasser Heakal; Alexander M Heberle; J Fielding Hejtmancik; Gudmundur Vignir Helgason; Vanessa Henkel; Marc Herb; Alexander Hergovich; Anna Herman-Antosiewicz; Agustín Hernández; Carlos Hernandez; Sergio Hernandez-Diaz; Virginia Hernandez-Gea; Amaury Herpin; Judit Herreros; Javier H Hervás; Daniel Hesselson; Claudio Hetz; Volker T Heussler; Yujiro Higuchi; Sabine Hilfiker; Joseph A Hill; William S Hlavacek; Emmanuel A Ho; Idy H T Ho; Philip Wing-Lok Ho; Shu-Leong Ho; Wan Yun Ho; G Aaron Hobbs; Mark Hochstrasser; Peter H M Hoet; Daniel Hofius; Paul Hofman; Annika Höhn; Carina I Holmberg; Jose R Hombrebueno; Chang-Won Hong Yi-Ren Hong; Lora V Hooper; Thorsten Hoppe; Rastislav Horos; Yujin Hoshida; I-Lun Hsin; Hsin-Yun Hsu; Bing Hu; Dong Hu; Li-Fang Hu; Ming Chang Hu; Ronggui Hu; Wei Hu; Yu-Chen Hu; Zhuo-Wei Hu; Fang Hua; Jinlian Hua; Yingqi Hua; Chongmin Huan; Canhua Huang; Chuanshu Huang; Chuanxin Huang; Chunling Huang; Haishan Huang; Kun Huang; Michael L H Huang; Rui Huang; Shan Huang; Tianzhi Huang; Xing Huang; Yuxiang Jack Huang; Tobias B Huber; Virginie Hubert; Christian A Hubner; Stephanie M Hughes; William E Hughes; Magali Humbert; Gerhard Hummer; James H Hurley; Sabah Hussain; Salik Hussain; Patrick J Hussey; Martina Hutabarat; Hui-Yun Hwang; Seungmin Hwang; Antonio Ieni; Fumiyo Ikeda; Yusuke Imagawa; Yuzuru Imai; Carol Imbriano; Masaya Imoto; Denise M Inman; Ken Inoki; Juan Iovanna; Renato V Iozzo; Giuseppe Ippolito; Javier E Irazoqui; Pablo Iribarren; Mohd Ishaq; Makoto Ishikawa; Nestor Ishimwe; Ciro Isidoro; Nahed Ismail; Shohreh Issazadeh-Navikas; Eisuke Itakura; Daisuke Ito; Davor Ivankovic; Saška Ivanova; Anand Krishnan V Iyer; José M Izquierdo; Masanori Izumi; Marja Jäättelä; Majid Sakhi Jabir; William T Jackson; Nadia Jacobo-Herrera; Anne-Claire Jacomin; Elise Jacquin; Pooja Jadiya; Hartmut Jaeschke; Chinnaswamy Jagannath; Arjen J Jakobi; Johan Jakobsson; Bassam Janji; Pidder Jansen-Dürr; Patric J Jansson; Jonathan Jantsch; Sławomir Januszewski; Alagie Jassey; Steve Jean; Hélène Jeltsch-David; Pavla Jendelova; Andreas Jenny; Thomas E Jensen; Niels Jessen; Jenna L Jewell; Jing Ji; Lijun Jia; Rui Jia; Liwen Jiang; Qing Jiang; Richeng Jiang; Teng Jiang; Xuejun Jiang; Yu Jiang; Maria Jimenez-Sanchez; Eun-Jung Jin; Fengyan Jin; Hongchuan Jin; Li Jin; Luqi Jin; Meiyan Jin; Si Jin; Eun-Kyeong Jo; Carine Joffre; Terje Johansen; Gail V W Johnson; Simon A Johnston; Eija Jokitalo; Mohit Kumar Jolly; Leo A B Joosten; Joaquin Jordan; Bertrand Joseph; Dianwen Ju; Jeong-Sun Ju; Jingfang Ju; Esmeralda Juárez; Delphine Judith; Gábor Juhász; Youngsoo Jun; Chang Hwa Jung; Sung-Chul Jung; Yong Keun Jung; Heinz Jungbluth; Johannes Jungverdorben; Steffen Just; Kai Kaarniranta; Allen Kaasik; Tomohiro Kabuta; Daniel Kaganovich; Alon Kahana; Renate Kain; Shinjo Kajimura; Maria Kalamvoki; Manjula Kalia; Danuta S Kalinowski; Nina Kaludercic; Ioanna Kalvari; Joanna Kaminska; Vitaliy O Kaminskyy; Hiromitsu Kanamori; Keizo Kanasaki; Chanhee Kang; Rui Kang; Sang Sun Kang; Senthilvelrajan Kaniyappan; Tomotake Kanki; Thirumala-Devi Kanneganti; Anumantha G Kanthasamy; Arthi Kanthasamy; Marc Kantorow; Orsolya Kapuy; Michalis V Karamouzis; Md Razaul Karim; Parimal Karmakar; Rajesh G Katare; Masaru Kato; Stefan H E Kaufmann; Anu Kauppinen; Gur P Kaushal; Susmita Kaushik; Kiyoshi Kawasaki; Kemal Kazan; Po-Yuan Ke; Damien J Keating; Ursula Keber; John H Kehrl; Kate E Keller; Christian W Keller; Jongsook Kim Kemper; Candia M Kenific; Oliver Kepp; Stephanie Kermorgant; Andreas Kern; Robin Ketteler; Tom G Keulers; Boris Khalfin; Hany Khalil; Bilon Khambu; Shahid Y Khan; Vinoth Kumar Megraj Khandelwal; Rekha Khandia; Widuri Kho; Noopur V Khobrekar; Sataree Khuansuwan; Mukhran Khundadze; Samuel A Killackey; Dasol Kim; Deok Ryong Kim; Do-Hyung Kim; Dong-Eun Kim; Eun Young Kim; Eun-Kyoung Kim; Hak-Rim Kim; Hee-Sik Kim; Jeong Hun Kim; Jin Kyung Kim; Jin-Hoi Kim; Joungmok Kim; Ju Hwan Kim; Keun Il Kim; Peter K Kim; Seong-Jun Kim; Scot R Kimball; Adi Kimchi; Alec C Kimmelman; Tomonori Kimura; Matthew A King; Kerri J Kinghorn; Conan G Kinsey; Vladimir Kirkin; Lorrie A Kirshenbaum; Sergey L Kiselev; Shuji Kishi; Katsuhiko Kitamoto; Yasushi Kitaoka; Kaio Kitazato; Richard N Kitsis; Josef T Kittler; Ole Kjaerulff; Peter S Klein; Thomas Klopstock; Jochen Klucken; Helene Knævelsrud; Roland L Knorr; Ben C B Ko; Fred Ko; Jiunn-Liang Ko; Hotaka Kobayashi; Satoru Kobayashi; Ina Koch; Jan C Koch; Ulrich Koenig; Donat Kögel; Young Ho Koh; Masato Koike; Sepp D Kohlwein; Nur M Kocaturk; Masaaki Komatsu; Jeannette König; Toru Kono; Benjamin T Kopp; Tamas Korcsmaros; Gözde Korkmaz; Viktor I Korolchuk; Mónica Suárez Korsnes; Ali Koskela; Janaiah Kota; Yaichiro Kotake; Monica L Kotler; Yanjun Kou; Michael I Koukourakis; Evangelos Koustas; Attila L Kovacs; Tibor Kovács; Daisuke Koya; Tomohiro Kozako; Claudine Kraft; Dimitri Krainc; Helmut Krämer; Anna D Krasnodembskaya; Carole Kretz-Remy; Guido Kroemer; Nicholas T Ktistakis; Kazuyuki Kuchitsu; Sabine Kuenen; Lars Kuerschner; Thomas Kukar; Ajay Kumar; Ashok Kumar; Deepak Kumar; Dhiraj Kumar; Sharad Kumar; Shinji Kume; Caroline Kumsta; Chanakya N Kundu; Mondira Kundu; Ajaikumar B Kunnumakkara; Lukasz Kurgan; Tatiana G Kutateladze; Ozlem Kutlu; SeongAe Kwak; Ho Jeong Kwon; Taeg Kyu Kwon; Yong Tae Kwon; Irene Kyrmizi; Albert La Spada; Patrick Labonté; Sylvain Ladoire; Ilaria Laface; Frank Lafont; Diane C Lagace; Vikramjit Lahiri; Zhibing Lai; Angela S Laird; Aparna Lakkaraju; Trond Lamark; Sheng-Hui Lan; Ane Landajuela; Darius J R Lane; Jon D Lane; Charles H Lang; Carsten Lange; Ülo Langel; Rupert Langer; Pierre Lapaquette; Jocelyn Laporte; Nicholas F LaRusso; Isabel Lastres-Becker; Wilson Chun Yu Lau; Gordon W Laurie; Sergio Lavandero; Betty Yuen Kwan Law; Helen Ka-Wai Law; Rob Layfield; Weidong Le; Herve Le Stunff; Alexandre Y Leary; Jean-Jacques Lebrun; Lionel Y W Leck; Jean-Philippe Leduc-Gaudet; Changwook Lee; Chung-Pei Lee; Da-Hye Lee; Edward B Lee; Erinna F Lee; Gyun Min Lee; He-Jin Lee; Heung Kyu Lee; Jae Man Lee; Jason S Lee; Jin-A Lee; Joo-Yong Lee; Jun Hee Lee; Michael Lee; Min Goo Lee; Min Jae Lee; Myung-Shik Lee; Sang Yoon Lee; Seung-Jae Lee; Stella Y Lee; Sung Bae Lee; Won Hee Lee; Ying-Ray Lee; Yong-Ho Lee; Youngil Lee; Christophe Lefebvre; Renaud Legouis; Yu L Lei; Yuchen Lei; Sergey Leikin; Gerd Leitinger; Leticia Lemus; Shuilong Leng; Olivia Lenoir; Guido Lenz; Heinz Josef Lenz; Paola Lenzi; Yolanda León; Andréia M Leopoldino; Christoph Leschczyk; Stina Leskelä; Elisabeth Letellier; Chi-Ting Leung; Po Sing Leung; Jeremy S Leventhal; Beth Levine; Patrick A Lewis; Klaus Ley; Bin Li; Da-Qiang Li; Jianming Li; Jing Li; Jiong Li; Ke Li; Liwu Li; Mei Li; Min Li; Min Li; Ming Li; Mingchuan Li; Pin-Lan Li; Ming-Qing Li; Qing Li; Sheng Li; Tiangang Li; Wei Li; Wenming Li; Xue Li; Yi-Ping Li; Yuan Li; Zhiqiang Li; Zhiyong Li; Zhiyuan Li; Jiqin Lian; Chengyu Liang; Qiangrong Liang; Weicheng Liang; Yongheng Liang; YongTian Liang; Guanghong Liao; Lujian Liao; Mingzhi Liao; Yung-Feng Liao; Mariangela Librizzi; Pearl P Y Lie; Mary A Lilly; Hyunjung J Lim; Thania R R Lima; Federica Limana; Chao Lin; Chih-Wen Lin; Dar-Shong Lin; Fu-Cheng Lin; Jiandie D Lin; Kurt M Lin; Kwang-Huei Lin; Liang-Tzung Lin; Pei-Hui Lin; Qiong Lin; Shaofeng Lin; Su-Ju Lin; Wenyu Lin; Xueying Lin; Yao-Xin Lin; Yee-Shin Lin; Rafael Linden; Paula Lindner; Shuo-Chien Ling; Paul Lingor; Amelia K Linnemann; Yih-Cherng Liou; Marta M Lipinski; Saška Lipovšek; Vitor A Lira; Natalia Lisiak; Paloma B Liton; Chao Liu; Ching-Hsuan Liu; Chun-Feng Liu; Cui Hua Liu; Fang Liu; Hao Liu; Hsiao-Sheng Liu; Hua-Feng Liu; Huifang Liu; Jia Liu; Jing Liu; Julia Liu; Leyuan Liu; Longhua Liu; Meilian Liu; Qin Liu; Wei Liu; Wende Liu; Xiao-Hong Liu; Xiaodong Liu; Xingguo Liu; Xu Liu; Xuedong Liu; Yanfen Liu; Yang Liu; Yang Liu; Yueyang Liu; Yule Liu; J Andrew Livingston; Gerard Lizard; Jose M Lizcano; Senka Ljubojevic-Holzer; Matilde E LLeonart; David Llobet-Navàs; Alicia Llorente; Chih Hung Lo; Damián Lobato-Márquez; Qi Long; Yun Chau Long; Ben Loos; Julia A Loos; Manuela G López; Guillermo López-Doménech; José Antonio López-Guerrero; Ana T López-Jiménez; Óscar López-Pérez; Israel López-Valero; Magdalena J Lorenowicz; Mar Lorente; Peter Lorincz; Laura Lossi; Sophie Lotersztajn; Penny E Lovat; Jonathan F Lovell; Alenka Lovy; Péter Lőw; Guang Lu; Haocheng Lu; Jia-Hong Lu; Jin-Jian Lu; Mengji Lu; Shuyan Lu; Alessandro Luciani; John M Lucocq; Paula Ludovico; Micah A Luftig; Morten Luhr; Diego Luis-Ravelo; Julian J Lum; Liany Luna-Dulcey; Anders H Lund; Viktor K Lund; Jan D Lünemann; Patrick Lüningschrör; Honglin Luo; Rongcan Luo; Shouqing Luo; Zhi Luo; Claudio Luparello; Bernhard Lüscher; Luan Luu; Alex Lyakhovich; Konstantin G Lyamzaev; Alf Håkon Lystad; Lyubomyr Lytvynchuk; Alvin C Ma; Changle Ma; Mengxiao Ma; Ning-Fang Ma; Quan-Hong Ma; Xinliang Ma; Yueyun Ma; Zhenyi Ma; Ormond A MacDougald; Fernando Macian; Gustavo C MacIntosh; Jeffrey P MacKeigan; Kay F Macleod; Sandra Maday; Frank Madeo; Muniswamy Madesh; Tobias Madl; Julio Madrigal-Matute; Akiko Maeda; Yasuhiro Maejima; Marta Magarinos; Poornima Mahavadi; Emiliano Maiani; Kenneth Maiese; Panchanan Maiti; Maria Chiara Maiuri; Barbara Majello; Michael B Major; Elena Makareeva; Fayaz Malik; Karthik Mallilankaraman; Walter Malorni; Alina Maloyan; Najiba Mammadova; Gene Chi Wai Man; Federico Manai; Joseph D Mancias; Eva-Maria Mandelkow; Michael A Mandell; Angelo A Manfredi; Masoud H Manjili; Ravi Manjithaya; Patricio Manque; Bella B Manshian; Raquel Manzano; Claudia Manzoni; Kai Mao; Cinzia Marchese; Sandrine Marchetti; Anna Maria Marconi; Fabrizio Marcucci; Stefania Mardente; Olga A Mareninova; Marta Margeta; Muriel Mari; Sara Marinelli; Oliviero Marinelli; Guillermo Mariño; Sofia Mariotto; Richard S Marshall; Mark R Marten; Sascha Martens; Alexandre P J Martin; Katie R Martin; Sara Martin; Shaun Martin; Adrián Martín-Segura; Miguel A Martín-Acebes; Inmaculada Martin-Burriel; Marcos Martin-Rincon; Paloma Martin-Sanz; José A Martina; Wim Martinet; Aitor Martinez; Ana Martinez; Jennifer Martinez; Moises Martinez Velazquez; Nuria Martinez-Lopez; Marta Martinez-Vicente; Daniel O Martins; Joilson O Martins; Waleska K Martins; Tania Martins-Marques; Emanuele Marzetti; Shashank Masaldan; Celine Masclaux-Daubresse; Douglas G Mashek; Valentina Massa; Lourdes Massieu; Glenn R Masson; Laura Masuelli; Anatoliy I Masyuk; Tetyana V Masyuk; Paola Matarrese; Ander Matheu; Satoaki Matoba; Sachiko Matsuzaki; Pamela Mattar; Alessandro Matte; Domenico Mattoscio; José L Mauriz; Mario Mauthe; Caroline Mauvezin; Emanual Maverakis; Paola Maycotte; Johanna Mayer; Gianluigi Mazzoccoli; Cristina Mazzoni; Joseph R Mazzulli; Nami McCarty; Christine McDonald; Mitchell R McGill; Sharon L McKenna; BethAnn McLaughlin; Fionn McLoughlin; Mark A McNiven; Thomas G McWilliams; Fatima Mechta-Grigoriou; Tania Catarina Medeiros; Diego L Medina; Lynn A Megeney; Klara Megyeri; Maryam Mehrpour; Jawahar L Mehta; Alfred J Meijer; Annemarie H Meijer; Jakob Mejlvang; Alicia Meléndez; Annette Melk; Gonen Memisoglu; Alexandrina F Mendes; Delong Meng; Fei Meng; Tian Meng; Rubem Menna-Barreto; Manoj B Menon; Carol Mercer; Anne E Mercier; Jean-Louis Mergny; Adalberto Merighi; Seth D Merkley; Giuseppe Merla; Volker Meske; Ana Cecilia Mestre; Shree Padma Metur; Christian Meyer; Hemmo Meyer; Wenyi Mi; Jeanne Mialet-Perez; Junying Miao; Lucia Micale; Yasuo Miki; Enrico Milan; Małgorzata Milczarek; Dana L Miller; Samuel I Miller; Silke Miller; Steven W Millward; Ira Milosevic; Elena A Minina; Hamed Mirzaei; Hamid Reza Mirzaei; Mehdi Mirzaei; Amit Mishra; Nandita Mishra; Paras Kumar Mishra; Maja Misirkic Marjanovic; Roberta Misasi; Amit Misra; Gabriella Misso; Claire Mitchell; Geraldine Mitou; Tetsuji Miura; Shigeki Miyamoto; Makoto Miyazaki; Mitsunori Miyazaki; Taiga Miyazaki; Keisuke Miyazawa; Noboru Mizushima; Trine H Mogensen; Baharia Mograbi; Reza Mohammadinejad; Yasir Mohamud; Abhishek Mohanty; Sipra Mohapatra; Torsten Möhlmann; Asif Mohmmed; Anna Moles; Kelle H Moley; Maurizio Molinari; Vincenzo Mollace; Andreas Buch Møller; Bertrand Mollereau; Faustino Mollinedo; Costanza Montagna; Mervyn J Monteiro; Andrea Montella; L Ruth Montes; Barbara Montico; Vinod K Mony; Giacomo Monzio Compagnoni; Michael N Moore; Mohammad A Moosavi; Ana L Mora; Marina Mora; David Morales-Alamo; Rosario Moratalla; Paula I Moreira; Elena Morelli; Sandra Moreno; Daniel Moreno-Blas; Viviana Moresi; Benjamin Morga; Alwena H Morgan; Fabrice Morin; Hideaki Morishita; Orson L Moritz; Mariko Moriyama; Yuji Moriyasu; Manuela Morleo; Eugenia Morselli; Jose F Moruno-Manchon; Jorge Moscat; Serge Mostowy; Elisa Motori; Andrea Felinto Moura; Naima Moustaid-Moussa; Maria Mrakovcic; Gabriel Muciño-Hernández; Anupam Mukherjee; Subhadip Mukhopadhyay; Jean M Mulcahy Levy; Victoriano Mulero; 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Per Nilsson; Shunbin Ning; Rituraj Niranjan; Hiroshi Nishimune; Mireia Niso-Santano; Ralph A Nixon; Annalisa Nobili; Clevio Nobrega; Takeshi Noda; Uxía Nogueira-Recalde; Trevor M Nolan; Ivan Nombela; Ivana Novak; Beatriz Novoa; Takashi Nozawa; Nobuyuki Nukina; Carmen Nussbaum-Krammer; Jesper Nylandsted; Tracey R O'Donovan; Seónadh M O'Leary; Eyleen J O'Rourke; Mary P O'Sullivan; Timothy E O'Sullivan; Salvatore Oddo; Ina Oehme; Michinaga Ogawa; Eric Ogier-Denis; Margret H Ogmundsdottir; Besim Ogretmen; Goo Taeg Oh; Seon-Hee Oh; Young J Oh; Takashi Ohama; Yohei Ohashi; Masaki Ohmuraya; Vasileios Oikonomou; Rani Ojha; Koji Okamoto; Hitoshi Okazawa; Masahide Oku; Sara Oliván; Jorge M A Oliveira; Michael Ollmann; James A Olzmann; Shakib Omari; M Bishr Omary; Gizem Önal; Martin Ondrej; Sang-Bing Ong; Sang-Ging Ong; Anna Onnis; Juan A Orellana; Sara Orellana-Muñoz; Maria Del Mar Ortega-Villaizan; Xilma R Ortiz-Gonzalez; Elena Ortona; Heinz D Osiewacz; Abdel-Hamid K Osman; Rosario Osta; Marisa S Otegui; 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Motomasa Tanaka; Daolin Tang; Jingfeng Tang; Tie-Shan Tang; Isei Tanida; Zhipeng Tao; Mohammed Taouis; Lars Tatenhorst; Nektarios Tavernarakis; Allen Taylor; Gregory A Taylor; Joan M Taylor; Elena Tchetina; Andrew R Tee; Irmgard Tegeder; David Teis; Natercia Teixeira; Fatima Teixeira-Clerc; Kumsal A Tekirdag; Tewin Tencomnao; Sandra Tenreiro; Alexei V Tepikin; Pilar S Testillano; Gianluca Tettamanti; Pierre-Louis Tharaux; Kathrin Thedieck; Arvind A Thekkinghat; Stefano Thellung; Josephine W Thinwa; V P Thirumalaikumar; Sufi Mary Thomas; Paul G Thomes; Andrew Thorburn; Lipi Thukral; Thomas Thum; Michael Thumm; Ling Tian; Ales Tichy; Andreas Till; Vincent Timmerman; Vladimir I Titorenko; Sokol V Todi; Krassimira Todorova; Janne M Toivonen; Luana Tomaipitinca; Dhanendra Tomar; Cristina Tomas-Zapico; Sergej Tomić; Benjamin Chun-Kit Tong; Chao Tong; Xin Tong; Sharon A Tooze; Maria L Torgersen; Satoru Torii; Liliana Torres-López; Alicia Torriglia; Christina G Towers; Roberto Towns; Shinya Toyokuni; Vladimir Trajkovic; Donatella Tramontano; Quynh-Giao Tran; Leonardo H Travassos; Charles B Trelford; Shirley Tremel; Ioannis P Trougakos; Betty P Tsao; Mario P Tschan; Hung-Fat Tse; Tak Fu Tse; Hitoshi Tsugawa; Andrey S Tsvetkov; David A Tumbarello; Yasin Tumtas; María J Tuñón; Sandra Turcotte; Boris Turk; Vito Turk; Bradley J Turner; Richard I Tuxworth; Jessica K Tyler; Elena V Tyutereva; Yasuo Uchiyama; Aslihan Ugun-Klusek; Holm H Uhlig; Marzena Ułamek-Kozioł; Ilya V Ulasov; Midori Umekawa; Christian Ungermann; Rei Unno; Sylvie Urbe; Elisabet Uribe-Carretero; Suayib Üstün; Vladimir N Uversky; Thomas Vaccari; Maria I Vaccaro; Björn F Vahsen; Helin Vakifahmetoglu-Norberg; Rut Valdor; Maria J Valente; Ayelén Valko; Richard B Vallee; Angela M Valverde; Greet Van den Berghe; Stijn van der Veen; Luc Van Kaer; Jorg van Loosdregt; Sjoerd J L van Wijk; Wim Vandenberghe; Ilse Vanhorebeek; Marcos A Vannier-Santos; Nicola Vannini; M Cristina Vanrell; Chiara Vantaggiato; Gabriele Varano; Isabel Varela-Nieto; 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Bo Wang; Chao-Yung Wang; Chen Wang; Chenran Wang; Chenwei Wang; Cun-Yu Wang; Dong Wang; Fangyang Wang; Feng Wang; Fengming Wang; Guansong Wang; Han Wang; Hao Wang; Hexiang Wang; Hong-Gang Wang; Jianrong Wang; Jigang Wang; Jiou Wang; Jundong Wang; Kui Wang; Lianrong Wang; Liming Wang; Maggie Haitian Wang; Meiqing Wang; Nanbu Wang; Pengwei Wang; Peipei Wang; Ping Wang; Ping Wang; Qing Jun Wang; Qing Wang; Qing Kenneth Wang; Qiong A Wang; Wen-Tao Wang; Wuyang Wang; Xinnan Wang; Xuejun Wang; Yan Wang; Yanchang Wang; Yanzhuang Wang; Yen-Yun Wang; Yihua Wang; Yipeng Wang; Yu Wang; Yuqi Wang; Zhe Wang; Zhenyu Wang; Zhouguang Wang; Gary Warnes; Verena Warnsmann; Hirotaka Watada; Eizo Watanabe; Maxinne Watchon; Anna Wawrzyńska; Timothy E Weaver; Grzegorz Wegrzyn; Ann M Wehman; Huafeng Wei; Lei Wei; Taotao Wei; Yongjie Wei; Oliver H Weiergräber; Conrad C Weihl; Günther Weindl; Ralf Weiskirchen; Alan Wells; Runxia H Wen; Xin Wen; Antonia Werner; Beatrice Weykopf; Sally P Wheatley; J Lindsay Whitton; 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Xi-Long Zheng; Yi Zheng; Zu-Guo Zheng; Boris Zhivotovsky; Qing Zhong; Ao Zhou; Ben Zhou; Cefan Zhou; Gang Zhou; Hao Zhou; Hong Zhou; Hongbo Zhou; Jie Zhou; Jing Zhou; Jing Zhou; Jiyong Zhou; Kailiang Zhou; Rongjia Zhou; Xu-Jie Zhou; Yanshuang Zhou; Yinghong Zhou; Yubin Zhou; Zheng-Yu Zhou; Zhou Zhou; Binglin Zhu; Changlian Zhu; Guo-Qing Zhu; Haining Zhu; Hongxin Zhu; Hua Zhu; Wei-Guo Zhu; Yanping Zhu; Yushan Zhu; Haixia Zhuang; Xiaohong Zhuang; Katarzyna Zientara-Rytter; Christine M Zimmermann; Elena Ziviani; Teresa Zoladek; Wei-Xing Zong; Dmitry B Zorov; Antonio Zorzano; Weiping Zou; Zhen Zou; Zhengzhi Zou; Steven Zuryn; Werner Zwerschke; Beate Brand-Saberi; X Charlie Dong; Chandra Shekar Kenchappa; Zuguo Li; Yong Lin; Shigeru Oshima; Yueguang Rong; Judith C Sluimer; Christina L Stallings; Chun-Kit Tong Journal: Autophagy Date: 2021-02-08 Impact factor: 13.391
Authors: Raymond A Sobel; Megan Albertelli; Julian R Hinojoza; Mary Jane Eaton; Kevin V Grimes; Edward Rubenstein Journal: J Neuropathol Exp Neurol Date: 2022-05-20 Impact factor: 3.148
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