Lindsay DeVorkin1, Nancy Erro Go2, Ying-Chen Claire Hou2, Annie Moradian3, Gregg B Morin4, Sharon M Gorski5. 1. The Genome Sciences Centre, British Columbia Cancer Agency, Vancouver, British Columbia V5Z 1L3, Canada Department of Molecular Biology and Biochemistry, Simon Fraser University, Burnaby, British Columbia V5A 1S6, Canada. 2. The Genome Sciences Centre, British Columbia Cancer Agency, Vancouver, British Columbia V5Z 1L3, Canada. 3. Department of Medical Genetics, University of British Columbia, Vancouver, British Columbia V5Z 1L3, Canada. 4. The Genome Sciences Centre, British Columbia Cancer Agency, Vancouver, British Columbia V5Z 1L3, Canada Department of Medical Genetics, University of British Columbia, Vancouver, British Columbia V5Z 1L3, Canada. 5. The Genome Sciences Centre, British Columbia Cancer Agency, Vancouver, British Columbia V5Z 1L3, Canada Department of Molecular Biology and Biochemistry, Simon Fraser University, Burnaby, British Columbia V5A 1S6, Canada sgorski@bcgsc.ca.
Abstract
Increasing evidence reveals that a subset of proteins participates in both the autophagy and apoptosis pathways, and this intersection is important in normal physiological contexts and in pathological settings. In this paper, we show that the Drosophila effector caspase, Drosophila caspase 1 (Dcp-1), localizes within mitochondria and regulates mitochondrial morphology and autophagic flux. Loss of Dcp-1 led to mitochondrial elongation, increased levels of the mitochondrial adenine nucleotide translocase stress-sensitive B (SesB), increased adenosine triphosphate (ATP), and a reduction in autophagic flux. Moreover, we find that SesB suppresses autophagic flux during midoogenesis, identifying a novel negative regulator of autophagy. Reduced SesB activity or depletion of ATP by oligomycin A could rescue the autophagic defect in Dcp-1 loss-of-function flies, demonstrating that Dcp-1 promotes autophagy by negatively regulating SesB and ATP levels. Furthermore, we find that pro-Dcp-1 interacts with SesB in a nonproteolytic manner to regulate its stability. These data reveal a new mitochondrial-associated molecular link between nonapoptotic caspase function and autophagy regulation in vivo.
Increasing evidence reveals that a subset of proteins participates in both the autophagy and apoptosis pathways, and this intersection is important in normal physiological contexts and in pathological settings. In this paper, we show that the Drosophila effector caspase, Drosophila caspase 1 (Dcp-1), localizes within mitochondria and regulates mitochondrial morphology and autophagic flux. Loss of Dcp-1 led to mitochondrial elongation, increased levels of the mitochondrial adenine nucleotide translocase stress-sensitive B (SesB), increased adenosine triphosphate (ATP), and a reduction in autophagic flux. Moreover, we find that SesB suppresses autophagic flux during midoogenesis, identifying a novel negative regulator of autophagy. Reduced SesB activity or depletion of ATP by oligomycin A could rescue the autophagic defect in Dcp-1 loss-of-function flies, demonstrating that Dcp-1 promotes autophagy by negatively regulating SesB and ATP levels. Furthermore, we find that pro-Dcp-1 interacts with SesB in a nonproteolytic manner to regulate its stability. These data reveal a new mitochondrial-associated molecular link between nonapoptotic caspase function and autophagy regulation in vivo.
Autophagy is a cellular self-digestion process in which long-lived proteins and organelles are engulfed in double-membrane vesicles called autophagosomes. After fusion with lysosomes to form autolysosomes, the cellular contents are degraded, and the resulting breakdown products, including constituents for ATP production and protein synthesis, are recycled back into the cell (Rabinowitz and White, 2010). Autophagic flux, which refers to the complete process of autophagy, occurs at basal levels and is also up-regulated in response to various cellular stresses, including nutrient deprivation (Filkins, 1970; Scott et al., 2004), chemotherapies (Bursch et al., 1996; Kanzawa et al., 2003; Høyer-Hansen and Jäättelä, 2008), and reactive oxygen species (Scherz-Shouval et al., 2007; Chen et al., 2009). As such, autophagy acts to remove toxic metabolites, harmful protein aggregates, and damaged organelles and provides a mechanism for energy production in instances of metabolic stress to promote cell survival. It is therefore not surprising that defects in autophagic flux have been implicated in several human diseases, including cancer (Kondo et al., 2005; Kimmelman, 2011) and neurodegeneration (Wong and Cuervo, 2010).The relationship between apoptosis and autophagy is complex, as core machinery components and signaling molecules of the pathways are interconnected (Eisenberg-Lerner et al., 2009). However, the molecular mechanisms governing these interactions are largely unknown. Several studies have begun to examine the multifunctional signaling molecules that take part in each pathway. For example, antiapoptotic Bcl-2 and Bcl-xL bind Beclin1, a core autophagy component of the class III phosphoinositide 3-kinase complex, and inhibit autophagy (Pattingre et al., 2005; Maiuri et al., 2007). Furthermore, the core autophagy protein Atg12 enhances mitochondrial apoptosis by binding to and inactivating antiapoptotic family members, including Bcl-2 and Mcl-1 (Rubinstein et al., 2011). Several studies have also revealed that core autophagy proteins undergo proteolytic processing, and in some cases, the newly generated fragment gains a novel proapoptotic role (Yousefi et al., 2006; Cho et al., 2009; Wirawan et al., 2010; Zhu et al., 2010).Studies using Drosophila melanogaster have also examined the complex relationship between autophagy and apoptosis. Overexpression of the autophagy gene Atg1 in the larval fat body, a nutrient storage organ analogous to the mammalian liver, induces apoptosis in a caspase-dependent manner (Scott et al., 2007). Degradation of larval tissues, including the salivary gland (Berry and Baehrecke, 2007) and the midgut (Denton et al., 2009), during development requires autophagy. Although these studies show that autophagy can lead to the induction of death as well as contribute to death-related processes, autophagy functions primarily as a cell survival mechanism in Drosophila in response to cellular stress. For example, JNK signaling in the intestinal epithelium and fat body stimulates autophagy gene transcription to promote cell survival during oxidative stress (Wu et al., 2009). Furthermore, autophagy is induced to high levels in the larval fat body (Scott et al., 2004) and the midgut (Wu et al., 2009) to remobilize nutrients and promote cell survival after starvation.The Drosophila ovary is also sensitive to nutritional cues. The ovary is made up of 15–20 ovarioles, each containing a series of developing egg chambers that arise from the germarium and progress through 14 well-defined stages. Each egg chamber is made up of 15 germline nurse cells and one oocyte surrounded by a layer of somatically derived follicle cells. Cell death in midstage egg chambers occurs sporadically and in response to environmental cues, including nutrient deprivation (Drummond-Barbosa and Spradling, 2001). Midstage egg chambers undergoing cell death are characterized by nurse cell nuclei condensation and fragmentation, engulfment of the nurse cell cytoplasm by the surrounding follicle cells and follicle cell death (Giorgi and Deri, 1976). Autophagy has been observed in degenerating midstage egg chambers (Hou et al., 2008; Nezis et al., 2009), and we previously showed that both cell death and autophagy are dependent on the effector caspaseDrosophila caspase-1 (Dcp-1; Song et al., 1997; Laundrie et al., 2003; Hou et al., 2008). However, whether autophagic flux occurs in response to starvation in nondegenerating and degenerating midstage egg chambers and the mechanism of Dcp-1–induced autophagy remain to be identified.In this study, we demonstrate that autophagic flux occurs in healthy and degenerating midstage egg chambers in response to starvation in a Dcp-1–dependent manner. We find that Dcp-1 localizes to the mitochondria under nutrient-rich conditions in which it functions to regulate mitochondrial network morphology and ATP levels. The proform of Dcp-1 interacts with the adenine nucleotide translocase (ANT) stress-sensitive B (SesB), a mitochondrial protein that functions to regulate ATP levels, in a nonproteolytic manner. SesB mutant analysis reveals a new role for SesB as a negative regulator of autophagic flux in Drosophila midstage egg chambers. Depletion of ATP or SesB loss-of-function flies can rescue the autophagy defect in Dcp-1 loss-of-function flies, demonstrating that SesB acts downstream of Dcp-1 in the regulation of autophagy. These data uncover a novel mechanism of caspase-mediated regulation of autophagy in vivo.
Results
Starvation-induced autophagic flux occurs during Drosophila midoogenesis and is regulated by Dcp-1
Using GFP-LC3 as a marker of autophagosomes, we previously showed that loss of Dcp-1 results in a reduction of starvation-induced autophagosome formation in vitro in Drosophilal(2)mbn cells and in vivo in degenerating midstage egg chambers (Hou et al., 2008). However, whether Dcp-1 affects autophagic flux, including the degradative completion of autophagy in the lysosome, remains to be identified. To test this, we first examined transgenic flies expressing a UASp-GFP-mCherry-DrAtg8a transgene specifically in the germline using the nosGAL4 driver. Under nonautophagy-inducing conditions, the dual-tagged Atg8a protein is diffuse throughout the cytoplasm and appears yellow (overlap of green and red). When autophagy is induced, Atg8a becomes lipidated and associates with the autophagosomal membrane where it fluoresces as yellow puncta. Once autophagosomes fuse with lysosomes, GFP fluorescence is quenched by acidic hydrolases, and the resulting autolysosome fluoresces red, signifying that autophagic flux has occurred (Nezis et al., 2010). Healthy egg chambers from flies conditioned on yeast paste (fed) showed diffuse yellow GFP-mCherry-DrAtg8a staining throughout the nurse cells (Fig. 1 A). After amino acid deprivation (starvation), we observed an increase in the percentage of autolysosomes (68 vs. 7% in fed conditions) in healthy nondegenerating midstage egg chambers (Fig. 1 B and Fig. S1 C), indicating that autophagic flux occurs in otherwise healthy egg chambers. In response to a cell death signal, nurse cell nuclei condense and fragment, follicle cells take up portions of the nurse cell cytoplasm, and this is followed by follicle cell death (Giorgi and Deri, 1976). In addition to the cell death phenotype, degenerating midstage egg chambers taking up nurse cell cytoplasm (Fig. 1 C) and those later in the degeneration process (Fig. 1 D) contained both autophagosomes and autolysosomes. In late degenerating midstage egg chambers, the GFP signal was lost, and the remaining follicle cells fluoresced red (Fig. 1 E), indicating that there may be a late stage acidification of the dying follicle cells. All together, these data show that autophagic flux occurs in the germline in response to starvation.
Figure 1.
Dcp-1 is necessary for autophagic flux during midoogenesis. GFP-mCherry-DrAtg8a was expressed in the germline using the nosGAL4 driver. Staining shows DNA, GFP, and mCherry. (A) UASp-GFP-mCherry-DrAtg8a/+;nosGAL4/+ flies conditioned on yeast paste had diffuse GFP-mCherry-DrAtg8a staining in midstage egg chambers. (B) Nondegenerating midstage egg chambers from starved flies contained autophagosomes (yellow) and autolysosomes (red). (C and D) Egg chambers early in the degeneration process showed follicle cells that take up portions of the nurse cell cytoplasm (C) followed by condensation and fragmentation of the nurse cell nuclei and further uptake of the nurse cell cytoplasm into follicle cells (D). (E) Late stage degenerating egg chambers lose all GFP staining and fluoresce red. (F) Fed Dcp-1 flies showed diffuse GFP-mCherry-DrAtg8a staining in the germline. (G) Starved Dcp-1 flies showed reduced autolysosomes in degenerating midstage egg chambers. (H and I) Fed flies overexpressing truncated Dcp-1 (tDcp-1) in the germline showed increased autophagosomes and autolysosomes in nondegenerating midstage egg chambers (H) and also contained degenerating midstage egg chambers that lose all GFP fluorescence and fluoresce red (I). Bars: (main images) 25 µm; (insets) 12.5 µm. Insets in A–I show diffuse cytoplasmic staining of Atg8a or autophagosomes and autolysosomes. (J and K) The percentages of autolysosomes (autolysosomes/total autophagic structures) were manually calculated in at least eight egg chambers for each genotype as indicated. Error bars represent the means ± SD. Statistical testing was performed using one-way ANOVA with a Dunnet post test (****, P < 0.0001) or a two-tailed Student’s t test (**, P < 0.005).
Dcp-1 is necessary for autophagic flux during midoogenesis. GFP-mCherry-DrAtg8a was expressed in the germline using the nosGAL4 driver. Staining shows DNA, GFP, and mCherry. (A) UASp-GFP-mCherry-DrAtg8a/+;nosGAL4/+ flies conditioned on yeast paste had diffuse GFP-mCherry-DrAtg8a staining in midstage egg chambers. (B) Nondegenerating midstage egg chambers from starved flies contained autophagosomes (yellow) and autolysosomes (red). (C and D) Egg chambers early in the degeneration process showed follicle cells that take up portions of the nurse cell cytoplasm (C) followed by condensation and fragmentation of the nurse cell nuclei and further uptake of the nurse cell cytoplasm into follicle cells (D). (E) Late stage degenerating egg chambers lose all GFP staining and fluoresce red. (F) Fed Dcp-1 flies showed diffuse GFP-mCherry-DrAtg8a staining in the germline. (G) Starved Dcp-1 flies showed reduced autolysosomes in degenerating midstage egg chambers. (H and I) Fed flies overexpressing truncated Dcp-1 (tDcp-1) in the germline showed increased autophagosomes and autolysosomes in nondegenerating midstage egg chambers (H) and also contained degenerating midstage egg chambers that lose all GFP fluorescence and fluoresce red (I). Bars: (main images) 25 µm; (insets) 12.5 µm. Insets in A–I show diffuse cytoplasmic staining of Atg8a or autophagosomes and autolysosomes. (J and K) The percentages of autolysosomes (autolysosomes/total autophagic structures) were manually calculated in at least eight egg chambers for each genotype as indicated. Error bars represent the means ± SD. Statistical testing was performed using one-way ANOVA with a Dunnet post test (****, P < 0.0001) or a two-tailed Student’s t test (**, P < 0.005).We next examined whether Dcp-1 regulates autophagic flux in the germline. Well-fed Dcp-1 loss-of-function flies (Dcp-1) expressing GFP-mCherry-DrAtg8a in the germline had diffuse yellow staining (Fig. 1, F and J). After starvation, degenerating midstage egg chambers from Dcp-1 flies, which are characterized by a premature loss of follicle cells and persisting nurse cell nuclei (Laundrie et al., 2003), contained a reduction in the percentage of autolysosomes compared with the control (Fig. 1, G [compare with D] and K). Nondegenerating midstage egg chambers from starved Dcp-1 flies also had reduced autophagic flux (Fig. S1), indicating that the reduction in autophagy in Dcp-1 flies is not simply caused by a lack of engulfment of dying nurse cells by follicle cells. To determine whether Dcp-1 is sufficient to induce autophagic flux, GFP-mCherry-Atg8a and an active form of Dcp-1 lacking its prodomain (tDcp-1) were expressed in the germline. We observed an increase in the percentage of autolysosomes in both nondegenerating (Fig. 1, H and J) and degenerating (Fig. 1 I) midstage egg chambers even in the absence of starvation.To confirm our in vivo findings, we examined the role of Dcp-1 in autophagic flux in vitro using a Drosophila S2 cell line stably expressing GFP-RFP-Atg8a. To validate the cell line, we first starved cells and observed a significant increase in autolysosomes that could be inhibited by addition of the late stage autophagy inhibitor Bafilomycin A1 (Fig. 2, A and B), as expected. Next, we used RNAi to knock down Rheb, a negative regulator of autophagy, or Atg7, a positive regulator of autophagy, and detected an increase and reduction in autolysosomes, respectively (Fig. 2, C and D). Dcp-1 RNAi resulted in a significant reduction in autolysosomes (Fig. 2, C and D), consistent with the Dcp-1 phenotype in midstage egg chambers, confirming a role for Dcp-1 as a positive regulator of autophagic flux.
Figure 2.
Dcp-1 regulates autophagic flux in vitro. (A) Drosophila S2 cells stably expressing GFP-RFP-Atg8a showed an increase in the percentage of cells containing two or more autolysosomes after starvation, which was blocked after Bafilomycin A1 (BafA1) treatment. At least 50 cells were manually quantitated in three independent experiments (n = 3). Statistical significance was determined using one-way ANOVA with a Dunnett post test (**, P < 0.01). (B) Representative images of S2-GFP-RFP-Atg8a cells after the indicated treatments. (C) S2-GFP-RFP-Atg8a cells were treated with dsRNAs and subjected to fed or starvation conditions as indicated. At least 50 cells were manually quantitated in three independent experiments (n = 3). Statistical significance was determined using one-way ANOVA with a Dunnett post test (**, P < 0.01; ***, P < 0.001; ****, P < 0.0001). (D) Representative images of S2-GFP-RFP-Atg8a cells after the indicated RNAi treatments. Error bars represent the means ± SD. Bars, 10 µm.
Dcp-1 regulates autophagic flux in vitro. (A) Drosophila S2 cells stably expressing GFP-RFP-Atg8a showed an increase in the percentage of cells containing two or more autolysosomes after starvation, which was blocked after Bafilomycin A1 (BafA1) treatment. At least 50 cells were manually quantitated in three independent experiments (n = 3). Statistical significance was determined using one-way ANOVA with a Dunnett post test (**, P < 0.01). (B) Representative images of S2-GFP-RFP-Atg8a cells after the indicated treatments. (C) S2-GFP-RFP-Atg8a cells were treated with dsRNAs and subjected to fed or starvation conditions as indicated. At least 50 cells were manually quantitated in three independent experiments (n = 3). Statistical significance was determined using one-way ANOVA with a Dunnett post test (**, P < 0.01; ***, P < 0.001; ****, P < 0.0001). (D) Representative images of S2-GFP-RFP-Atg8a cells after the indicated RNAi treatments. Error bars represent the means ± SD. Bars, 10 µm.We also investigated whether Dcp-1 regulates starvation-induced autophagy in the larval fat body using LysoTracker red (LTR), an acidotropic dye that labels both autolysosomes and lysosomes. After 1 h of starvation, fat bodies from larvae overexpressing Dcp-1 contained increased LTR and Atg8a puncta, whereas control larvae contained low LTR levels and diffuse Atg8a staining (Fig. S2, A and B). Fat bodies from 4-h-starved wild-type and Dcp-1 flies had high LTR and Atg8a puncta (Fig. S2, C and D), indicating that although Dcp-1 overexpression can enhance the autophagic response, Dcp-1 is not required for starvation-induced autophagy in the fat body.
Dcp-1 is required for the degradation of Ref(2)P after starvation
Ref(2)P, the Drosophila homologue of p62 (Nezis et al., 2008), is a substrate of autophagy and was shown to be a marker of autophagic activity (Nezis et al., 2010; Bartlett et al., 2011). Therefore, we used Ref(2)P analyses to confirm that Dcp-1 is a positive regulator of autophagic flux. Compared with fed wild-type flies (Fig. 3 A), nutrient-deprived flies had reduced Ref(2)P in follicle cells and nurse cells (Fig. 3 B), and Western blot analysis of wild-type ovaries revealed that the level of Ref(2)P was reduced after starvation (Fig. 3 C). Ovaries from fed or starved Atg7 mutant flies showed an accumulation of Ref(2)P (Fig. 3, C and D). It was reported that starvation itself leads to transcriptional activation of Ref(2)P (Érdi et al., 2012), and this is likely why we see an even further increase in Ref(2)P levels after starvation in Atg7 flies. Compared with starved wild-type flies, degenerating midstage egg chambers from starved Dcp-1 flies contained increased levels of Ref(2)P (Fig. 3 E), and Western blot analysis of whole ovaries confirmed that Ref(2)P failed to be completely degraded after starvation (Fig. 3 F). The effect of Dcp-1 on Ref(2)P levels is modest compared with Atg7: we found that Ref(2)P accumulates only in degenerating midstage egg chambers of Dcp-1 flies after starvation. The variability in the levels of Ref(2)P, as shown in Fig. 3 F, is most likely caused by the extent of the persisting or “undead” egg chambers present in the samples. In contrast to Atg7 flies, Dcp-1 does not affect basal autophagy. Altogether, these data show that Dcp-1 is a positive regulator of starvation-induced autophagic flux during Drosophila midoogenesis.
Figure 3.
Ref(2)P analyses confirm that Dcp-1 is required for autophagic flux in ovaries. Staining shows DNA, Ref(2)P, and Armadillo. Zoomed insets show Ref(2)P staining. (A) Nondegenerating midstage egg chambers from fed w flies showed Ref(2)P staining in follicle cells and nurse cells. (B) Starved w flies contained degenerating midstage egg chambers with reduced Ref(2)P. (C) A representative Western blot of ovaries from w and Atg7 flies subjected to fed or starvation conditions for 4 d. Ref(2)P was detected by immunoblotting. Actin served as a loading control. Densitometry was performed to quantitate Ref(2)P protein levels relative to actin. Graph represents ± SD from five independent experiments (n = 5). Statistical significance was determined using a two-tailed Student’s t test. *, P = 0.004 for fed samples; *, P = 0.008 for starved samples. (D) Starved Atg7 flies showed an accumulation of Ref(2)P in the follicle cells and nurse cells of degenerating midstage egg chambers. (E) Starved Dcp-1 flies contained increased levels of Ref(2)P in degenerating midstage egg chambers. (F) A representative Western blot of ovaries from w and Dcp-1 flies that were subjected to fed or starvation conditions for 4 d. Ref(2)P was detected by immunoblotting. Actin served as a loading control. Densitometry was performed to quantitate Ref(2)P protein levels relative to actin. Graph represents ± SD from five independent experiments (n = 5). Statistical significance was determined using a two-tailed Student’s t test. *, P = 0.03. Bars: (main images) 25 µm; (zoomed images) 10 µm.
Ref(2)P analyses confirm that Dcp-1 is required for autophagic flux in ovaries. Staining shows DNA, Ref(2)P, and Armadillo. Zoomed insets show Ref(2)P staining. (A) Nondegenerating midstage egg chambers from fed w flies showed Ref(2)P staining in follicle cells and nurse cells. (B) Starved w flies contained degenerating midstage egg chambers with reduced Ref(2)P. (C) A representative Western blot of ovaries from w and Atg7 flies subjected to fed or starvation conditions for 4 d. Ref(2)P was detected by immunoblotting. Actin served as a loading control. Densitometry was performed to quantitate Ref(2)P protein levels relative to actin. Graph represents ± SD from five independent experiments (n = 5). Statistical significance was determined using a two-tailed Student’s t test. *, P = 0.004 for fed samples; *, P = 0.008 for starved samples. (D) Starved Atg7 flies showed an accumulation of Ref(2)P in the follicle cells and nurse cells of degenerating midstage egg chambers. (E) Starved Dcp-1 flies contained increased levels of Ref(2)P in degenerating midstage egg chambers. (F) A representative Western blot of ovaries from w and Dcp-1 flies that were subjected to fed or starvation conditions for 4 d. Ref(2)P was detected by immunoblotting. Actin served as a loading control. Densitometry was performed to quantitate Ref(2)P protein levels relative to actin. Graph represents ± SD from five independent experiments (n = 5). Statistical significance was determined using a two-tailed Student’s t test. *, P = 0.03. Bars: (main images) 25 µm; (zoomed images) 10 µm.
Dcp-1 localizes to the mitochondria
To elucidate the mechanism by which Dcp-1 mediates autophagic flux, we first determined the subcellular location of Dcp-1 in Drosophilal(2)mbn cells by immunostaining with an antibody to Dcp-1 (Fig. S3; Tenev et al., 2005). We observed colocalization between Dcp-1 and the mitochondrial markers ATPsynthase-α (ATPsyn-α; Fig. 4 A) and MitoTracker red (Fig. 4 B) but did not observe colocalization between Dcp-1 and markers for the endoplasmic reticulum or cis-Golgi (Fig. S3, A and B). Dcp-1 was also found to colocalize with β-Tubulin (Fig. S3 C). To confirm that Dcp-1 is located at the mitochondria, subcellular fractionation was performed on l(2)mbn cells subjected to nutrient-rich medium or 6 h of starvation (Fig. 4 C). Purity of the fractions was determined using Tubulin as a cytosolic (Fig. 4 C, abbreviated as C) marker and ATPsyn-α, voltage-dependent anion channel (VDAC), and cytochrome c as the membrane-enriched (Fig. 4 C, abbreviated as M) markers. Using a previously described antibody (Fig. S3 E; Laundrie et al., 2003), we found that the proform (zymogen) of Dcp-1 was located only in the membrane-enriched fraction in nutrient-rich and starvation conditions, whereas the processed p10 subunit of Dcp-1 was found in both the membrane and cytosolic fractions (Fig. 4 C). Similar results were obtained after subcellular fractionation of ovaries (Fig. 4 D). To determine whether Dcp-1 is located inside the mitochondria or is associated with the surface of the outer mitochondrial membrane, a proteinase K protection assay was performed with or without hypotonic disruption of the mitochondria. Mitochondrial proteins within the mitochondria are resistant to proteinase K treatment, whereas proteins located on the surface of the outer mitochondrial membrane, but not embedded within the lipid bilayer of mitochondria, are sensitive to proteinase K (Smith et al., 1994; Setoguchi et al., 2006). VDAC, an embedded outer mitochondrial membrane protein, and ATPsyn-α, a mitochondrial matrix protein, remained intact upon proteinase K treatment as expected but were digested by proteinase K after hypotonic disruption of the mitochondria (Fig. 4 E). In addition, Pink1, a mitochondrial protein associated with the outer mitochondrial membrane, was degraded after proteinase K treatment as expected (Fig. 4 F). Examination of Dcp-1 showed that it was digested only after hypotonic disruption of the mitochondria, indicating that Dcp-1 is internalized within the mitochondria (Fig. 4, E and F). We speculate that the proform of Dcp-1 translocates into the mitochondria where a fraction of it is processed into its active form, and this active form either remains in the mitochondria or translocates back into the cytosol. Together, these data demonstrate that pro–Dcp-1 localizes within mitochondria.
Figure 4.
Dcp-1 is partially localized within mitochondria. (A and B) l(2)mbn cells were labeled with antibodies to Dcp-1 and ATPsyn-α (A) or MitoTracker red (MTR; B). Merged images show colocalization between Dcp-1 and the mitochondria. Boxes represent zoomed images. Bars: (main images) 5 µm; (zoomed images) 1.25 µm. (C) Western blot from l(2)mbn cells subjected to nutrient-rich or starvation conditions for 6 h. Cells were separated into cytosolic (C) and mitochondrial enriched (M) fractions. (D) Ovaries from fed w flies were separated into cytosolic and membrane-enriched fractions and probed with antibodies to VDAC, Tubulin, ATPsyn-α, and Dcp-1. (E and F) Intact and lysed mitochondria (E) or intact mitochondria isolated from l(2)mbn cells (F) were treated with proteinase K (PK). The effects of proteinase K treatment were assessed by antibodies to VDAC, ATPsyn-α, Pink1, and Dcp-1. (G) Control and Dcp-1 RNAi–treated cells were subjected to nutrient-rich or starvation conditions and stained with NAO. Mean fluorescence was measured by flow cytometry. Graph represents ± SEM of three independent experiments (n = 3).
Dcp-1 is partially localized within mitochondria. (A and B) l(2)mbn cells were labeled with antibodies to Dcp-1 and ATPsyn-α (A) or MitoTracker red (MTR; B). Merged images show colocalization between Dcp-1 and the mitochondria. Boxes represent zoomed images. Bars: (main images) 5 µm; (zoomed images) 1.25 µm. (C) Western blot from l(2)mbn cells subjected to nutrient-rich or starvation conditions for 6 h. Cells were separated into cytosolic (C) and mitochondrial enriched (M) fractions. (D) Ovaries from fed w flies were separated into cytosolic and membrane-enriched fractions and probed with antibodies to VDAC, Tubulin, ATPsyn-α, and Dcp-1. (E and F) Intact and lysed mitochondria (E) or intact mitochondria isolated from l(2)mbn cells (F) were treated with proteinase K (PK). The effects of proteinase K treatment were assessed by antibodies to VDAC, ATPsyn-α, Pink1, and Dcp-1. (G) Control and Dcp-1 RNAi–treated cells were subjected to nutrient-rich or starvation conditions and stained with NAO. Mean fluorescence was measured by flow cytometry. Graph represents ± SEM of three independent experiments (n = 3).
Loss of Dcp-1 alters morphology of the mitochondrial network
To examine a potential role of Dcp-1 at the mitochondria, we first analyzed whether loss of Dcp-1 alters mitochondrial mass. No changes in mitochondrial mass as detected by 10-N-nonyl acridine orange (NAO), a fluorescent dye that binds mitochondrial cardiolipin independently of mitochondrial membrane potential (Maftah et al., 1989), were detected in nutrient-rich or starvation conditions (Fig. 4 G). Next, we determined whether loss of Dcp-1 alters mitochondrial morphology. Mitochondria were labeled with ATPsyn-α and were scored as having a fragmented, a normal (containing both short and elongated mitochondria), or an elongated morphology (Fig. 5 A). The majority of control cells in nutrient-rich media contained mitochondria with a normal morphology, and starvation led to an increase in the percentage of cells with elongated mitochondria (Fig. 5 B). Treatment with Dcp-1 RNAi resulted in a significant increase in cells that contained elongated mitochondria in both nutrient-rich and starvation media (Fig. 5 B). Given that the changes observed in mitochondrial morphology after Dcp-1 RNAi were not associated with changes in mitochondrial mass under the conditions tested (Fig. 4 G) suggests that Dcp-1 may play a role in maintaining the mitochondrial network under fed and starvation conditions.
Figure 5.
Loss of Dcp-1 promotes mitochondrial elongation. (A) l(2)mbn cells were labeled with the ATPsyn-α, and mitochondrial morphology was scored as fragmented, normal, or elongated. (B) Cells were treated with control or Dcp-1 dsRNA and subjected to nutrient-rich media or 1 h of starvation. Quantifications represent the percentage of cells with elongated mitochondria divided by the total number of cells examined. At least 100 cells were examined manually in three independent experiments (n = 3). Error bars represent the mean ± SD. Statistical significance was determined using one-way ANOVA with a Bonferroni post test (*, P < 0.05; **, P < 0.01). (C) Mitochondrial targeted GFP (mitoGFP) was expressed in the germline using the nosGAL4 driver. Staining shows mitoGFP, Armadillo, and DNA. (D) Mitochondria were scored as healthy (H), clustered (C), or elongated and overly connected (E). All of mitochondria from fed UASp-mitoGFP/+;nosGAL4/+ flies were scored as healthy. n = 15 egg chambers manually scored. (E) mitoGFP was expressed in Dcp-1 flies using the nosGAL4 driver. (F) 54% of egg chambers from UASp-mitoGFP/+;Dcp-1 flies contained elongated mitochondria, 39% contained mitochondria that were scored as healthy, and 7% contained clustered mitochondria. n = 28 egg chambers manually scored. Bars: (A) 5 µm; (C and E, main images) 25 µm; (C and E, zoomed images) 10 µm.
Loss of Dcp-1 promotes mitochondrial elongation. (A) l(2)mbn cells were labeled with the ATPsyn-α, and mitochondrial morphology was scored as fragmented, normal, or elongated. (B) Cells were treated with control or Dcp-1 dsRNA and subjected to nutrient-rich media or 1 h of starvation. Quantifications represent the percentage of cells with elongated mitochondria divided by the total number of cells examined. At least 100 cells were examined manually in three independent experiments (n = 3). Error bars represent the mean ± SD. Statistical significance was determined using one-way ANOVA with a Bonferroni post test (*, P < 0.05; **, P < 0.01). (C) Mitochondrial targeted GFP (mitoGFP) was expressed in the germline using the nosGAL4 driver. Staining shows mitoGFP, Armadillo, and DNA. (D) Mitochondria were scored as healthy (H), clustered (C), or elongated and overly connected (E). All of mitochondria from fed UASp-mitoGFP/+;nosGAL4/+ flies were scored as healthy. n = 15 egg chambers manually scored. (E) mitoGFP was expressed in Dcp-1 flies using the nosGAL4 driver. (F) 54% of egg chambers from UASp-mitoGFP/+;Dcp-1 flies contained elongated mitochondria, 39% contained mitochondria that were scored as healthy, and 7% contained clustered mitochondria. n = 28 egg chambers manually scored. Bars: (A) 5 µm; (C and E, main images) 25 µm; (C and E, zoomed images) 10 µm.To determine whether Dcp-1 alters mitochondrial morphology in vivo, we expressed mitochondrial targeting GFP (mitoGFP) in the germline of Dcp-1 flies. All fed control flies contained short, tubular mitochondria that were dispersed throughout the entire nurse cell (Fig. 5 C) and were scored as healthy (Fig. 5 D, abbreviated as H). Starvation induces a series of mitochondrial events in degenerating midstage egg chambers, including mitochondrial remodeling and clustering, uptake by the follicle cells, and finally, degradation within the follicle cells (Tanner et al., 2011). Fed Dcp-1 flies expressing mitoGFP in the germline contained mitochondria with an altered morphology even in the absence of starvation. 54% of midstage egg chambers from Dcp-1 flies contained mitochondria that were elongated and overly connected (Fig. 5, E and F, abbreviated as E), whereas only 39% of midstage egg chambers contained mitochondria that were healthy (Fig. 5 F, abbreviated as H). To control for the different genetic backgrounds between wild-type and Dcp-1 flies with respect to the mitochondrial phenotypes, Dcp-1 was overexpressed in the germline of Dcp-1 flies to determine whether the mitochondrial phenotype could be rescued. Indeed, 94% of midstage egg chambers from Dcp-1 flies overexpressing wild-type Dcp-1 showed healthy mitochondria compared with only 33% of midstage egg chambers from Dcp-1 flies (Fig. S4, A–C), indicating that the mitochondrial phenotype is caused by the Dcp-1 mutation. These data demonstrate that Dcp-1 plays a role in the regulation of mitochondrial network morphology even in the absence of a starvation signal, underscoring a novel nonapoptotic role of an effector caspase in regulating mitochondrial dynamics under both fed and starvation conditions.
High ATP levels in Dcp-1 flies suppress autophagic flux
Loss of Dcp-1 promotes elongation of the mitochondrial network, and mitochondrial elongation has been shown to sustain ATP levels after starvation to promote cell survival (Gomes et al., 2011). In addition, the cellular energy sensor AMP-activated protein kinase is activated when the ratio of ATP/AMP falls, for example, during periods of starvation (Salt et al., 1998; Gleason et al., 2007), thus stimulating energy producing pathways such as autophagy (Kim et al., 2011). Therefore, we determined whether Dcp-1 also alters ATP levels as a mechanism to induce autophagic flux. Cells treated with Dcp-1 RNAi showed a significant increase in ATP levels within 4 h of starvation (Fig. 6 A), suggesting that at least under starvation in vitro, the elongated mitochondrial phenotype in Dcp-1 RNAi-treated cells is associated with increased ATP levels. To confirm this in vivo, we examined ovaries from wild-type and Dcp-1 flies subjected to fed or starvation conditions and found ATP levels to be significantly increased in ovaries of Dcp-1 flies under both conditions tested (Fig. 6 B). We reasoned that the increased ATP levels in Dcp-1 flies may inhibit autophagic flux after starvation. Reduction of ATP with oligomycin A, an inhibitor of the mitochondrial ATP synthase, induces autophagy in the IPLB-LdFB insect cell line (Tettamanti et al., 2006), and so, we tested whether oligomycin A would induce autophagy in Drosophila ovaries. Although oligomycin A did not alter Ref(2)P levels under fed conditions, ovaries from starved Dcp-1 flies treated with oligomycin A showed a significant reduction in Ref(2)P protein compared with those treated with DMSO (Fig. 6 C). In addition, starved oligomycin A–treated Dcp-1 flies expressing GFP-mCherry-DrAtg8a in the germline showed an increase in the percentage of autolysosomes in degenerating midstage egg chambers compared with those treated with DMSO (red puncta; Fig. 6 E), whereas we observed no additional increase in the percentage of autolysosomes in starved control flies treated with oligomycin A (Fig. 6 D). This suggests that high ATP levels are sufficient to block autophagic flux in Dcp-1 flies after starvation. Collectively, our data demonstrate that Dcp-1 controls autophagic flux by a mechanism involving the regulation of the mitochondrial network and maintenance of ATP levels.
Figure 6.
Dcp-1 alters ATP levels that in turn regulate autophagy. (A) Total cellular ATP levels were measured in l(2)mbn cells treated with control or Dcp-1 dsRNA. Data represent ± SEM of three independent experiments (n = 3). Statistical significance was determined using a two-tailed Students t test (*, P = 0.02). (B) Total cellular ATP levels were measured in ovaries from fed or starved w8 and Dcp-1 flies. Data represent ± SEM of five independent experiments (n = 5). Statistical significance was determined using a two-tailed Student’s t test (**, P = 0.014; ***, P < 0.001). (C) Fed or starved w and Dcp-1 flies were treated with DMSO or 25 µg/ml oligomycin A, and Ref(2)P levels were assessed by immunoblot analysis. Actin served as a loading control. Densitometry was performed to quantitate protein levels relative to actin. Graph represents ± SD from three independent experiments (n = 3). Statistical significance was determined using a two-tailed Student’s t test (*, P = 0.02). (D and E) Control UASp-GFP-mCherry-DrAtg8a/+;nosGAL4/+ flies (D) and Dcp-1 flies (E) were subjected to starvation conditions supplemented with DMSO or 25 µg/ml oligomycin A. Bars, 25 µm. Quantifications show percentage of autolysosomes (autolysosomes/total autophagic structures). At least eight egg chambers were manually quantitated per genotype per condition (n = 8). Statistical testing was determined using a two-tailed Student’s t test. ***, P = 0.0002.
Dcp-1 alters ATP levels that in turn regulate autophagy. (A) Total cellular ATP levels were measured in l(2)mbn cells treated with control or Dcp-1 dsRNA. Data represent ± SEM of three independent experiments (n = 3). Statistical significance was determined using a two-tailed Students t test (*, P = 0.02). (B) Total cellular ATP levels were measured in ovaries from fed or starved w8 and Dcp-1 flies. Data represent ± SEM of five independent experiments (n = 5). Statistical significance was determined using a two-tailed Student’s t test (**, P = 0.014; ***, P < 0.001). (C) Fed or starved w and Dcp-1 flies were treated with DMSO or 25 µg/ml oligomycin A, and Ref(2)P levels were assessed by immunoblot analysis. Actin served as a loading control. Densitometry was performed to quantitate protein levels relative to actin. Graph represents ± SD from three independent experiments (n = 3). Statistical significance was determined using a two-tailed Student’s t test (*, P = 0.02). (D and E) Control UASp-GFP-mCherry-DrAtg8a/+;nosGAL4/+ flies (D) and Dcp-1 flies (E) were subjected to starvation conditions supplemented with DMSO or 25 µg/ml oligomycin A. Bars, 25 µm. Quantifications show percentage of autolysosomes (autolysosomes/total autophagic structures). At least eight egg chambers were manually quantitated per genotype per condition (n = 8). Statistical testing was determined using a two-tailed Student’s t test. ***, P = 0.0002.
Dcp-1 negatively regulates the levels of the ANT SesB
Dcp-1 regulates levels of SesB but SesB is not a direct target of Dcp-1’s proteolytic activity. (A) A representative Western blot showing SesB and ATPsyn-α levels from fed or starved l(2)mbn cells treated with control or Dcp-1 RNAi. Actin served as a loading control. Densitometry was performed to quantitate protein levels relative to actin. Graphs represent ± SD from three independent experiments (n = 3). Statistical significance was determined using a two-tailed Student’s t test (*, P < 0.05). (B) A representative Western blot of ovaries from fed or starved w or Dcp-1 flies. SesB and ATPsyn-α were detected by immunoblotting. Actin served as a loading control. Densitometry was performed to quantitate protein levels relative to actin. Graphs represent ± SD from three independent experiments (n = 3). Statistical significance was determined using a two-tailed Student’s t test (*, P < 0.05). (C) Purified catalytically active Dcp-1FL, but not catalytically inactive Dcp-1C
SesB is a negative regulator of autophagic flux and interacts genetically with Dcp-1
The loss of SesB after starvation suggests that SesB may negatively regulate autophagy. To test this, we examined ovaries from SesB hypomorphic flies (SesB) that were shown to have reduced ANT activity (Rikhy et al., 2003). Consistent with this previous study, ovaries from SesB flies had reduced ATP levels compared with ovaries from wild-type flies (Fig. S5 C). Although fed wild-type flies rarely contain degenerating midstage egg chambers (Table S1), fed SesB flies contained an increase in degenerating midstage egg chambers (Table S1) that had increased LTR staining (Fig. S5 F) and reduced Ref(2)P (Fig. 8, A and B). Loss of SesB resulted in a similar phenotype in the larval fat body (Fig. S2). In addition, overexpression of GFP-mCherry-DrAtg8a in the germline of fed SesB flies revealed an increase in the percentage of autolysosomes in both nondegenerating (Fig. 8, C [left] and D) and degenerating (Fig. 8 C, right) midstage egg chambers, confirming that there is increased autophagic flux in SesB flies. Degenerating midstage egg chambers from SesB flies also stained positively for TUNEL (Fig. 8 E), suggesting that SesB is normally required to suppress autophagic flux and DNA fragmentation during Drosophila oogenesis.
Figure 8.
SesB hypomorphic flies have an enhanced autophagy phenotype, and epistasis analysis indicates that SesB acts downstream of Dcp-1. (A) Ovaries from fed SesB flies show reduced Ref(2)P staining in degenerating midstage egg chamber (arrow). (B) Ovaries from fed w and SesB were analyzed by Western blotting using Ref(2)P. Actin served as a loading control. Results are representative of three independent experiments (n = 3). (C) SesB flies expressing GFP-mCherry-DrAtg8a in the germline showed increased autophagosomes and autolysosomes in nondegenerating (left) and degenerating (right) midstage egg chambers. Insets show autophagosomes and autolysosomes (left) and autolysosomes (right) in SesB midstage egg chambers. (D) Quantitation of percentages of autolysosomes (autolysosomes/total autophagic structures) in nondegenerating ovaries from fed w and SesB flies. 10 egg chambers were manually examined per genotype. Error bars represent the means ± SD. Statistical significance was determined using a two-tailed Student’s t test (***, P < 0.0001). (E) Degenerating midstage egg chambers (arrows) from fed SesB flies are TUNEL positive. (F) Degenerating midstage egg chambers from starved control SesB flies contained persisting nurse cell nuclei and increased Ref(2)P. n = 117 ovarioles examined. Box represents zoomed image. (G) Degenerating midstage egg chambers from fed SesB flies contained condensed and fragmented nurse cell nuclei and low levels of Ref(2)P. Box represents zoomed image. n = 156 ovarioles examined. (H) In response to starvation, Dcp-1 acts to negatively regulate the levels of SesB. SesB is a negative regulator of autophagy, and reduced SesB levels mediated by Dcp-1 lead to decreased ATP and induction of autophagic flux. Bars: (A, C [main images], E, F [main images], and G [main images]) 25 µm; (C, insets) 12.5 µm; (F and G [zoomed images]) 10 µm.
SesB hypomorphic flies have an enhanced autophagy phenotype, and epistasis analysis indicates that SesB acts downstream of Dcp-1. (A) Ovaries from fed SesB flies show reduced Ref(2)P staining in degenerating midstage egg chamber (arrow). (B) Ovaries from fed w and SesB were analyzed by Western blotting using Ref(2)P. Actin served as a loading control. Results are representative of three independent experiments (n = 3). (C) SesB flies expressing GFP-mCherry-DrAtg8a in the germline showed increased autophagosomes and autolysosomes in nondegenerating (left) and degenerating (right) midstage egg chambers. Insets show autophagosomes and autolysosomes (left) and autolysosomes (right) in SesB midstage egg chambers. (D) Quantitation of percentages of autolysosomes (autolysosomes/total autophagic structures) in nondegenerating ovaries from fed w and SesB flies. 10 egg chambers were manually examined per genotype. Error bars represent the means ± SD. Statistical significance was determined using a two-tailed Student’s t test (***, P < 0.0001). (E) Degenerating midstage egg chambers (arrows) from fed SesB flies are TUNEL positive. (F) Degenerating midstage egg chambers from starved control SesB flies contained persisting nurse cell nuclei and increased Ref(2)P. n = 117 ovarioles examined. Box represents zoomed image. (G) Degenerating midstage egg chambers from fed SesB flies contained condensed and fragmented nurse cell nuclei and low levels of Ref(2)P. Box represents zoomed image. n = 156 ovarioles examined. (H) In response to starvation, Dcp-1 acts to negatively regulate the levels of SesB. SesB is a negative regulator of autophagy, and reduced SesB levels mediated by Dcp-1 lead to decreased ATP and induction of autophagic flux. Bars: (A, C [main images], E, F [main images], and G [main images]) 25 µm; (C, insets) 12.5 µm; (F and G [zoomed images]) 10 µm.To determine the epistatic relationship between Dcp-1 and SesB, we examined fed and nutrient-deprived SesB double mutant flies. Because of the high levels of SesB in Dcp-1 flies, we reasoned that by reducing SesB in the Dcp-1 background, a SesB phenotype would result. Degenerating midstage egg chambers from nutrient-deprived control SesB flies contained persisting nurse cell nuclei and an accumulation of Ref(2)P (Fig. 8 F). In contrast, ovarioles from fed SesB flies arrested during midoogenesis, and these midstage egg chambers contained condensed and fragmented nurse cell nuclei and reduced Ref(2)P levels (Fig. 8 G), similar to the SesB phenotype. These data place Dcp-1 upstream of SesB, suggesting that Dcp-1 may promote autophagy by inhibiting SesB activity. All together, these data demonstrate that SesB is a novel negative regulator of autophagic flux during Drosophila midoogenesis, and its levels are reduced after starvation in a Dcp-1–dependent manner.
Discussion
Our results reveal that starvation-induced autophagic flux occurs in both midstage egg chambers that have not entered the degeneration process as well as in those that are undergoing cell death. Furthermore, we find that the effector caspaseDcp-1 is required for autophagic flux in degenerating midstage egg chambers in addition to its role in cell death. We find that one mechanism of Dcp-1–induced autophagic flux is mediated through SesB. In humans, there are four mitochondrial ANT isoforms, each with a tissue-specific distribution and different roles in apoptosis. ANT1 and ANT3 were proposed to be proapoptotic, whereas ANT2 and ANT4 were shown to be antiapoptotic (Brenner et al., 2011). However, the roles of mammalianANT proteins in autophagy have yet to be characterized. Our data show that reduced Dcp-1 leads to increased levels of SesB protein in fed and starvation conditions during Drosophila oogenesis and in Drosophila cultured cells. We detected no significant change in SesB transcript levels in fed conditions or after 4 h of starvation, but a significant increase was observed in cells after 2 h of starvation. This finding suggests that a transcription-related mechanism may play some role in the observed cellular response but is not sufficient to account for all of the observed changes in protein levels. Although Dcp-1 does not cleave SesB, the proform of Dcp-1 interacts with SesB, and we predict that this interaction regulates the stability of SesB. We find that SesB is required to suppress autophagic flux during midoogenesis even under nutrient-rich conditions, and reduction of SesB in Dcp-1 flies rescues the autophagic defect after starvation. This is the first study to our knowledge showing that an ANT functions as a negative regulator of autophagy.The Drosophila genome encodes seven caspases, and to date, only the initiator caspase Dronc and the effector caspase Drice have been shown to localize to the mitochondria (Dorstyn et al., 2002). In mammalian cells, caspases have been detected at the mitochondria during apoptosis (Krajewski et al., 1999; Susin et al., 1999; Chandra and Tang, 2003); however, the role of caspases at the mitochondria, especially under nonapoptotic conditions, is poorly understood. Our results demonstrate that Dcp-1 localizes to the mitochondria where it functions to maintain the mitochondrial network morphology. Under nutrient-rich conditions, nondegenerating midstage egg chambers from Dcp-1 flies contained mitochondria that appeared elongated and overly connected, and ovaries contained increased ATP levels, indicating that Dcp-1 normally functions to negatively regulate mitochondrial dynamics and ATP levels. Consistent with our findings, overexpression of the caspase inhibitor p35 in the amnioserosa suppressed the transition of mitochondria from a tubular to a fragmented state during delamination (Muliyil et al., 2011), further suggesting that inhibition of caspases hinders normal mitochondrial dynamics.Dcp-1 acts to finely tune the apoptotic process, and cell death only occurs when caspase activity reaches a certain apoptotic threshold (Florentin and Arama, 2012). Effector caspases involved in nonapoptotic processes may be restricted in time or space to regulate caspase activity (Kaplan et al., 2010; Florentin and Arama, 2012). As Dcp-1 functions not only in autophagy and apoptosis but also at the mitochondria to regulate mitochondrial morphology and ATP levels, one question that remains is to how the activity of Dcp-1 is regulated. As Dcp-1 has autocatalytic activity (Song et al., 1997), perhaps Dcp-1 is sequestered in mitochondria to prevent its full activation. Mitochondrial localized mammalian pro–Caspase 3 and 9 are S-nitrosylated in their catalytic active site, leading to the inhibition of their activity (Mannick et al., 2001). Perhaps mitochondrial Dcp-1 is also S-nitrosylated, serving to limit Dcp-1’s activity. In addition, mammalianHsp60 and Hsp10 were shown to interact with mitochondrial localized pro–Caspase 3 in which they function to accelerate pro–Caspase 3 activation after the induction of apoptosis (Samali et al., 1999). Perhaps Dcp-1 associates with Drosophila Hsp60 or Hsp10 in the mitochondria to regulate its mitochondrial related functions. However, further studies are required to identify upstream regulators of Dcp-1 that regulate its mitochondrial, autophagic, and apoptotic functions.Effector caspases are the main executioners of apoptotic cell death; however, it is becoming increasingly evident that caspases have nonapoptotic functions in differentiation, proliferation, cytokine production, and cell survival (Kuranaga and Miura, 2007; Galluzzi et al., 2012). For example, Caspase 3 was shown to regulate tumor cell repopulation in vitro and in vivo (Huang et al., 2011), and it was also shown to be required for skeletal muscle (Fernando et al., 2002) and macrophage differentiation (Sordet et al., 2002). In Drosophila, the initiator caspase Dronc maintains neural stem cell homeostasis by binding to Numb in a noncatalytic, nonapoptotic manner to regulate its activity (Ouyang et al., 2011). In addition, Dcp-1 is required for neuromuscular degeneration in a nonapoptotic manner (Keller et al., 2011). Our results show that Dcp-1 also has a nonapoptotic role during oogenesis, in which it is required to maintain mitochondrial physiology under basal conditions. Loss of Dcp-1 alters this physiology, leading to increased SesB and ATP levels that in part prevent the induction of autophagic flux after starvation. These data support the notion that caspases play a much more diverse role than previously known and that the underlying mechanisms should be better understood to appreciate the full impact of apoptosis pathway modulation for treatment in human pathologies.
Materials and methods
Fly strains
w was used at the wild-type control strain in this study. Other fly strains used are as follows: nanos-GAL4::VP16 (abbreviated as nosGAL4, a driver containing the Gal4-VP16 transactivator under the control of the nanos promoter; Rørth, 1998), UASp-mitoGFP (expresses the COX VIII mitochondrial targeting sequence fused to EGFP under the UASp promoter; Cox and Spradling, 2003), Dcp-1 (contains a 40-bp partial P element insertion in the coding region of Dcp-1, resulting in a frame shift in Dcp-1 and an in-frame stop codon within the 40-bp insertion; Laundrie et al., 2003), and UASp-FL-Dcp-1 (drives expression of full-length Dcp-1 under the UASp promoter; Peterson et al., 2003) were gifts from K. McCall (Boston University, Boston, MA). Atg7 (P element excision removing CG5335 and exons 5 and 6 and most of exon 4 from Atg7) and Atg7 (P element excision removing the transcription and translation start sites and the majority of the Atg7 coding region) were gifts from T. Neufeld (University of Minnesota, Minneapolis MN; Juhász et al., 2007). UASp-GFP-mCherry-DrAtg8a (drives expression of GFP-mCherry-DrAtg8a under the UASp promoter) was a gift from T.E. Rusten (Centre for CancerBiomedicine, Oslo University Hospital, Montebello, Oslo, Norway; Nezis et al., 2010), and SesB hypomorphic flies, which contain a glutamate to lysine change at amino acid 266 that disrupts normal SesB activity, were obtained from the Bloomington Stock Center (stock 27590).
Cell culture conditions
Drosophilal(2)mbn cells were grow in Schneider’s medium (Invitrogen) supplemented with 10% FBS in 25-cm2 suspension cell flasks (Sarstedt) at 25°C. Drosophila S2-RFP-GFP-Atg8a cells were grown in ESF921 medium (Expression Systems) in the presence of 50 µg/ml Zeocin. All experiments were performed 3–4 d after passage.
Construction of RFP-GFP-ATG8a plasmid and creation of S2-RFP-GFP-Atg8a stable cell line
ATG8a was amplified using the primers 5′-TGACCTAGCTAGATCTAAGTTCCAATACAAGGAGGA-3′ and 5′-TGACCTAGCTGAATTCTTAGTTAATTTTGGCCATGCC-3′. Atg8a was cloned into the BglII–EcoRI sites of mRFP-EGFP-LC3 (Kimura et al., 2007). The cytomegalovirus promoter from this construct was removed using AseI–NheI digestion and replaced with the actin promoter amplified from pAFW (Drosophila Genomics Resource Center) using the primers 5′-TGACGATCGCATTAATCAGCATGCAATTCTATATTCT-3′ and 5′-TGACGATCGCGCTAGCGGCCTCGATATCTGGATCCGG-3′. The Pactin-RFP-GFP-ATG8a fragment (AseI–MluI digest) was then subcloned in the HindIII site of the previously described p2ZOp2F vector (Hegedus et al., 1998), which contains Zeocin as a selection agent for transfection in Drosophila cell lines. For transfections, 1 µg Pactin-RFP-GFP-ATG8a was added to 10 µl Cellfectin (Invitrogen) plus 100 µl Grace’s medium (Invitrogen) and incubated for ≥30 min. 3.75 × 106 S2 cells in 400 µl Grace’s media were incubated with transfection medium overnight. 1 ml ESF921 medium (Expression Systems) was added back to the cells, and the cells were incubated for an additional 3 d before adding Zeocin at a concentration of 0.6–0.8 mg/ml. The media were replaced every 4 d until the negative control showed 0% viability (∼3 wk). Transfected cells were maintained in ESF921 + 0.1 mg/ml Zeocin.
Double-stranded RNA (dsRNA) synthesis
Each PCR primer for RT-PCR was designed to contain a 5′ T7 RNA polymerase binding site (5′-TAATACGACTCACTATAGG-3′) followed by sequences specific for the target gene. The ampicillin resistance gene was used as a control dsRNA and was amplified using the primers 5′-TAATACGACTCACTATAGGATTGGACTACGATACGGGAGGGCTT-3′ and 5′-TAATACGACTCACTATAGGATTGGGCTATGTGGCGCGGTATTAT-3′. Dcp-1 was amplified using the primers 5′-TAATACGACTCACTATAGGACAAAAGCTGGCTGAGAAGC-3′ and 5′-TAATACGACTCACTATAGGCAGCCATTATAAAGCTGCCC-3′. The PCR products were generated by RT-PCR using SuperScript One-Step RT-PCR with Platinum Taq (Invitrogen). RT-PCR products were ethanol precipitated and used as a template for in vitro transcription reactions using T7 RiboMAX Express RNAi System (Promega). Quality of the RNA was analyzed by gel electrophoresis. dsRNA was quantitated using PicoGreen and adjusted to 200–400 ng/µl with nuclease-free water.
RNAi
For RNAi, cells were washed and resuspended in ESF921 medium to a concentration of 2 × 106 cells/ml. 333 µl of adjusted cells was plated in each well of a 24-well plate. 5–10 µg dsRNA was added per well and incubated at 25°C for 1 h. After incubation, 667 µl Schneider’s + 10% FBS was added back to each well and was incubated for an additional 72 h at 25°C.
Immunofluorescence experiments
Flies were conditioned on wet yeast paste for 2 d (fed) and then transferred to a vial containing 10% sucrose for 4 d for amino acid starvation. Ovaries were dissected in PBS and fixed with 4% paraformaldehyde. Ovaries were washed with PBS-T (PBS + 0.3% Triton X-100), permeabilized with 0.5% Triton X-100, and blocked with 2% BSA in PBS-T. For in vitro experiments, 200 µl cells was plated into an 8-well CC2-coated chamber slide and incubated for ≥30 min to let the cells adhere. For starvation treatments, media were replaced with 2 mg/ml glucose/PBS. For MitoTracker experiments, 500 nm MitoTracker red CMXRos (Invitrogen) was added to each well and incubated for 30 min in the dark at 25°C. Media were removed and fixed with 4% paraformaldehyde for 20 min. Cells were washed with PBS-T and permeabilized with 0.5% Triton X-100.Primary antibodies included rabbit anti-Ref(2)P (1:5,000; T.E. Rusten), mouse anti-Armadillo (1:100; N2 7A1; Developmental Studies Hybridoma Bank) mouse anti–ATPsyn-α (1:500; MitoSciences), guinea pig anti–Dcp-1 (1:500;Tenev et al., 2005), mouse anti–β-Tubulin (1:1,000; E7; Developmental Studies Hybridoma Bank), mouse anti–protein disulfide isomerase (1:100; Abcam), and rabbit anti-GM130 (1:100; Abcam) were diluted in 0.5% BSA + PBS-T. Secondary antibodies included Alexa Fluor 488– and Alexa Fluor 546–conjugated antibodies (1:1,000; Invitrogen). For Draq5 DNA stain, Draq5 was diluted in PBS (1:500) with 100 µg/ml RNase A for 10 min at room temperature. Samples were mounted with SlowFade gold antifade reagent (Invitrogen) and viewed with a microscope (Confocal C1; Nikon) equipped with a Plan Apochromat 60×/1.45 NA oil immersion objective (Nikon) or a 20×/0.75 NA objective lens. Images were acquired at room temperature using EZ-C1 version 3.00 software (Nikon). Images were scanned with the same pinhole and laser brightness settings. Brightness and contrast were adjusted using Photoshop (CS4; Adobe) and was applied to the whole image.
LTR and TUNEL analysis
For LTR staining of ovaries, ovaries from fed, and amino acid–starved flies were dissected in PBS and incubated in 50 µm LTR DND-99 for 3 min, washed three times with PBS, and fixed with 4% paraformaldehyde for 20 min. Ovaries were washed three times with PBS-T (PBS + 0.3% Triton X-100), incubated in 1:500 Draq5 + 100 µg/ml RNase A for 10 min at room temperature, and mounted in SlowFade gold reagent. For LTR of fat bodies, second instar larvae were transferred to a cornmeal/dextrose fly food agar plate supplemented with yeast paste 48 h after hatching. 12–24 h later, fed larvae were dissected or were transferred to a plate containing 20% sucrose for 1–4 h before dissecting. Fat bodies were dissected in PBS and transferred to 0.8 µm LTR (Invitrogen) for 5 min at room temperature in the dark. Tissues were then incubated with 1:500 Draq5 + 100 µg/ml RNase A for 10 min at room temperature, washed three times in PBS, and mounted with SlowFade at room temperature.For TUNEL analysis, ovaries were dissected in PBS and fixed with 4% paraformaldehyde. Ovaries were washed two times with PBS, permeabilized with 0.2% Triton X-100 for 5 min, and washed two additional times with PBS. The TUNEL assay was performed using the fluorometric TUNEL system (DeadEnd; Promega) according to the manufacturer’s instructions. Ovaries were incubated with 1:500 Draq5 + 100 µg/ml RNase A for 10 min at room temperature and viewed by confocal microscopy.
Mitochondrial scoring
For in vitro experiments, mitochondrial morphology was first assessed under basal conditions by two independent researchers, and a classification scheme (fragmented, normal, and elongated) was devised and agreed upon by both researchers. For in vivo experiments, mitochondria were assessed in both fed and nutrient-deprived control flies, and a scoring scheme (healthy, clustered, or elongated and overly connected) was devised based on similar observations made in healthy and degenerating midstage egg chambers (scored as healthy, normally degenerating, or abnormal) described in Tanner et al. (2011).
Protein extraction and Western blot analysis
For ovary lysates, ovaries were dissected and placed immediately on dry ice. Cell and ovary lysates were extracted using radioimmunoprecipitation assay lysis buffer (Santa Cruz Biotechnology, Inc.) plus complete protease inhibitors (Roche). Protein was quantitated using the Bicinchoninic Acid Protein Assay (Thermo Fisher Scientific). Proteins were separated on a 4–12% NuPAGE Bis-Tris gel (Invitrogen) and transferred to polyvinylidene fluoride membranes. Membranes were blocked in milk or Odyssey blocking buffer and incubated in primary antibodies overnight at 4°C. Primary antibodies included rabbit anti-Ref(2)P (1:10,000), mouse anti-actin (1:500; JLA20; Developmental Studies Hybridoma Bank), mouse anti-Tubulin (1:1,000; E7), mouse anti–ATPsyn-α (1:1,000), mouse anti-Porin (1:1,000; MitoSciences), mouse anti-ANT (1:500; MitoSciences), rabbit anti–Dcp-1 (1:500; Laundrie et al., 2003), guinea pig anti–Dcp-1 (1:500; Tenev et al., 2005), rabbit anti-Pink1 (1:500; Abcam), and rabbit anti-Atg8a (1:1,000; Barth et al., 2011). Membranes were incubated with HRP-conjugated secondary antibodies or infrared-labeled secondary antibodies and were detected using the ECL Enhanced Western Blotting System (GE Healthcare) or the Odyssey System (LI-COR Biosciences). Densitometry was performed using ImageQuant 5.1 software (GE Healthcare).
Isolation of crude mitochondrial and cytosolic fractions
Approximately 5 × 107 cells were collected by centrifugation at 800 rpm for 10 min, resuspended in cold SEM-P (10 mM MOPS, pH 7.5, 320 mM sucrose, and 1 mM EDTA with complete protease inhibitor cocktail [Roche]), and ground using a dounce homogenizer. Lysates were centrifuged twice at 3,000 rpm to remove cell debris, and supernatants were collected. The membrane fraction (pellet) was separated from the cytosolic fraction (supernatant) by centrifugation at 12,000 rpm. The pellets were washed once with 500 µl SEM-P and finally resuspended in 50 µl SEM-P. Protein concentrations were determined using the Bicinchoninic Acid Protein Assay. Aliquots of 50 µg protein were either spun down (membrane fraction) or TCA precipitated (cytosolic fraction) and analyzed by Western blotting.
Proteinase K protection assay
For mitochondrial lysis, mitochondria were resuspended in the appropriate amount of swelling buffer (50 mM Tris, pH 7.5) for 30 min on ice with vigorous vortexing. Intact and lysed mitochondria were incubated in 20 µg/ml proteinase K (Roche). Proteinase K was inactivated by adding PMSF (Fluka) to a final concentration of 1 mM. Intact mitochondria were spun down at 4°C and 12,000 rpm for 20 min while lysed samples were TCA precipitated.
Oligomycin A treatment
3–5-d-old flies were transferred to a vial containing wet yeast paste supplemented with 200 µl of 25-µg/ml Oligomycin A or DMSO added directly to the top of the yeast paste. After 2 d of treatment, flies were transferred to a vial containing a Kimwipe soaked with 10% sucrose supplemented with 25 µg/ml Oligomycin A or DMSO for 4 d.
Mitochondrial mass analysis and determination of ATP levels
RNAi-treated cells were transferred from Schneider + 10% FBS to 2 mg/ml glucose/PBS starvation media plus 10 µg dsRNA for 1–24 h. For mitochondrial mass measurements, cells were incubated with 10 µM NAO for 10 min at 25°C in the dark. Cells were resuspended and put on ice to be analyzed by flow cytometry (FACSCalibur; BD). A minimum of 30,000 cells was acquired for triplicate samples per experiment. The mean fluorescence was analyzed using FlowJo Software version 5.7.2 (Tree Star, Inc.).ATP levels from l(2)mbn cells or Drosophila ovaries were measured using the ATP Determination Kit (Invitrogen) according to the manufacturer’s recommendations. Luminescence was measured using a plate reader (Wallac 1420 Victor; PerkinElmer).
Generation of constructs and in vitro synthesis
Drice (Tenev et al., 2005) was PCR amplified using primers containing AttB1 and AttB2 sequences. SesB was amplified from a full-length cDNA construct (Drosophila Genomics Resource Center) using primers containing AttB1 and AttB2 sequences. PCR products were cloned into the pDONR221 Gateway Entry Vector (Life Technologies) and were sequenced verified. The entry clones were then shuttled into the pEXP2-DEST and pEXP1-DEST expression vectors, respectively, for in vitro translation experiments. Sequences used for plasmid construction can be found in Table S1. SesB and Drice were synthesized using the Expressway Mini Expression Module (Invitrogen) according to the manufacturer’s instructions. 1 µg of template DNA was used for every 100 µl of synthesis reaction in a 6-h reaction. PCR primers were used as follows: Drice AttB1, 5′-GGGGACAAGTTTGTACAAAAAAGCAGGCTTCACCATGGACGCCACTAACAATGGAGAAT-3′; Drice AttB2, 5′-GGGGACCACTTTGTACAAGAAAGCTGGGTCTCAAACCCGTCCGGCTGGT-3′; SesBAttB1, 5′-GGGGACAAGTTTGTACAAAAAAGCAGGCTTCACCATGGGCAAGGATTTCGATGCTGTT-3′; and SesBAttB2, 5′-GGGGACCACTTTGTACAAGAAAGCTGGGTCCAAGACCTTCTTGATCTCAT-3′.
Transfection and purification of Dcp-1 and in vitro cleavage assays
RNAi-treated cells were subjected to nutrient-full or starvation conditions for 2 or 4 h and were collected and pelleted at 850 rpm for 5 min. Cell pellets were lysed in 1 ml TRIZOL (Invitrogen), and total RNA was extracted according to the manufacturer’s instructions. RNA was treated with DNase, and QRT-PCR was performed using the One-Step SYBR green RT-PCR reagent kit (Applied Biosystems) on a 7900 Sequence Detection System (Applied Biosystems). Expression levels were calculated using the comparative threshold method with Drosophilarp49 as the reference gene. QRT-PCR primers are as follows: rp49, 5′-ATACAGGCCCAAGATCGTGA-3′ and 5′-GCACTCTGTTGTCGATACCCTT-3′, and SesB, 5′-AAGGATTTCGATGCTGTTGG-3′ and 5′-CTCCTTTGGAATGCGGATAA-3′.
IP and MS/MS analysis
For large-scale IP experiments, 96 ml V5–Dcp-1C196A or V5 vector control–transfected l(2)mbn cells were centrifuged at 800 rpm for 10 min. Nutrient-full medium was replaced with either new 10% FBS/Schneider medium (fed) or 2 mg/ml glucose/PBS for 2-h starvation treatment. Cells were centrifuged at 800 rpm for 10 min and cross-linked with 0.25% paraformaldehyde at 25°C for 40 min. 1.25 M glycine (final = 0.125 M) was added and incubated for 5 min at room temperature to stop the cross-linking reaction. Samples were then centrifuged at 800 rpm for 10 min and lysed (20 mM Tris, pH 7.5, 150 mM NaCl, 1 mM EDTA, 1% NP-40, 10 mM β-glycerophosphate, 2 mM sodium orthovanadate, 1 mM 4-(2-aminoethyl) benzenesulfonyl fluoride hydrochloride, 10 µg/ml pepstatin A, 10 µg/ml leupeptin, and 10 µg/ml aprotinin). Cells were disrupted by passing through a 21-gauge syringe five times, and lysates were incubated at 4°C for 30 min. Cells were spun down, and supernatants were incubated with a 50% slurry of Sepharose 4B (Sigma-Aldrich) for 1 h at 4°C. Sepharose 4B was removed by centrifugation, and supernatants were incubated with a 50% slurry of anti-V5 affinity agarose resin for 3 h at 4°C. Anti-V5 resins were recovered by centrifugation and washed 5× with cold lysis buffer and 2× lysis buffer with 500 mM NaCl. Bound proteins were eluted by 0.5 M formic acid. Eluates were boiled for 20 min at 95°C to reverse the formaldehyde cross-links. Eluates were then vacuum dried, resuspended in protein sample buffer (Invitrogen), and separated by SDS-PAGE using a 10% NuPAGE gel (Invitrogen) and MES buffer. Protein bands were visualized with the colloidal Coomassie stain, and each lane was cut into 16 equal sections. Gel slices were transferred into a 96-well plate, reduced with 10 mM DTT, S-alkylated with 100 mM iodoacetamide, and then subjected to in-gel trypsin digestion with 20 µl of 20-ng/µl trypsin per well overnight at 37°C. Peptide mixtures were subjected to liquid chromatography MS/MS analysis on a Finnigan LCQ (PTRL West) or a 4000 QTRAP (Applied Biosystems) ion trap mass spectrometer via reversed phase HPLC nanoelectrospray ionization. All MS–MS spectra were queried against the Drosophila Ensembl sequence databases (Flicek et al., 2014) using the Mascot (Matrix Science) or X!Tandem (Craig and Beavis, 2004) algorithms. Candidate interacting proteins were identified as described in Mead et al. (2010). In brief, putative interacting proteins were identified by at least two peptides each having an X!Tandem log(e) score less than −3 and were identified in at least two experimental samples (V5–Dcp-1C
Statistics
In each graph, data represent ± SEM or SD of n independent experiments. As indicated in the legends, statistical significance was calculated by analysis of variance (ANOVA) plus a Dunnett or Bonferroni post test, or a two-tailed Student’s t test between the indicated samples was used. P-values are shown in the legends.
Online supplemental material
Fig. S1 shows that Dcp-1 flies have reduced autolysosomes in nondegenerating midstage egg chambers after starvation. Fig. S2 shows LTR and Atg8a antibody staining in fat bodies of Dcp-1, CG-GAL4/+;UASDcp-1/+, SesB, and control flies. Fig. S3 shows a lack of colocalization between Dcp-1 and the ER or Golgi but does show localization between Dcp-1 and β-Tubulin. Fig. S4 shows that overexpression of Dcp-1 can rescue the Dcp-1 mitochondrial phenotype. Fig. S5 shows SesB QRT-PCR analysis, FLAG-SesB localization to mitochondria, and that ovaries from SesB flies have reduced ATP and contain increased LTR staining in degenerating midstage egg chambers. Table S1 shows quantification of TUNEL-positive germaria and midstage egg chambers. Table S2 shows identification of SesB by MS. Online supplemental material is available at http://www.jcb.org/cgi/content/full/jcb.201303144/DC1.
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Audrey Esclatine; Mafalda Escobar-Henriques; Eeva-Liisa Eskelinen; Lucile Espert; Makandjou-Ola Eusebio; Gemma Fabrias; Cinzia Fabrizi; Antonio Facchiano; Francesco Facchiano; Bengt Fadeel; Claudio Fader; Alex C Faesen; W Douglas Fairlie; Alberto Falcó; Bjorn H Falkenburger; Daping Fan; Jie Fan; Yanbo Fan; Evandro F Fang; Yanshan Fang; Yognqi Fang; Manolis Fanto; Tamar Farfel-Becker; Mathias Faure; Gholamreza Fazeli; Anthony O Fedele; Arthur M Feldman; Du Feng; Jiachun Feng; Lifeng Feng; Yibin Feng; Yuchen Feng; Wei Feng; Thais Fenz Araujo; Thomas A Ferguson; Álvaro F Fernández; Jose C Fernandez-Checa; Sonia Fernández-Veledo; Alisdair R Fernie; Anthony W Ferrante; Alessandra Ferraresi; Merari F Ferrari; Julio C B Ferreira; Susan Ferro-Novick; Antonio Figueras; Riccardo Filadi; Nicoletta Filigheddu; Eduardo Filippi-Chiela; Giuseppe Filomeni; Gian Maria Fimia; Vittorio Fineschi; Francesca Finetti; Steven Finkbeiner; Edward A Fisher; Paul B Fisher; Flavio Flamigni; Steven J Fliesler; Trude H Flo; Ida Florance; Oliver Florey; Tullio Florio; Erika Fodor; Carlo Follo; Edward A Fon; Antonella Forlino; Francesco Fornai; Paola Fortini; Anna Fracassi; Alessandro Fraldi; Brunella Franco; Rodrigo Franco; Flavia Franconi; Lisa B Frankel; Scott L Friedman; Leopold F Fröhlich; Gema Frühbeck; Jose M Fuentes; Yukio Fujiki; Naonobu Fujita; Yuuki Fujiwara; Mitsunori Fukuda; Simone Fulda; Luc Furic; Norihiko Furuya; Carmela Fusco; Michaela U Gack; Lidia Gaffke; Sehamuddin Galadari; Alessia Galasso; Maria F Galindo; Sachith Gallolu Kankanamalage; Lorenzo Galluzzi; Vincent Galy; Noor Gammoh; Boyi Gan; Ian G Ganley; Feng Gao; Hui Gao; Minghui Gao; Ping Gao; Shou-Jiang Gao; Wentao Gao; Xiaobo Gao; Ana Garcera; Maria Noé Garcia; Verónica E Garcia; Francisco García-Del Portillo; Vega Garcia-Escudero; Aracely Garcia-Garcia; Marina Garcia-Macia; Diana García-Moreno; Carmen Garcia-Ruiz; Patricia García-Sanz; Abhishek D Garg; Ricardo Gargini; Tina Garofalo; Robert F Garry; Nils C Gassen; Damian Gatica; Liang Ge; Wanzhong Ge; Ruth Geiss-Friedlander; Cecilia Gelfi; Pascal Genschik; Ian E Gentle; Valeria Gerbino; Christoph Gerhardt; Kyla Germain; Marc Germain; David A Gewirtz; Elham Ghasemipour Afshar; Saeid Ghavami; Alessandra Ghigo; Manosij Ghosh; Georgios Giamas; Claudia Giampietri; Alexandra Giatromanolaki; Gary E Gibson; Spencer B Gibson; Vanessa Ginet; Edward Giniger; Carlotta Giorgi; Henrique Girao; Stephen E Girardin; Mridhula Giridharan; Sandy Giuliano; Cecilia Giulivi; Sylvie Giuriato; Julien Giustiniani; Alexander Gluschko; Veit Goder; Alexander Goginashvili; Jakub Golab; David C Goldstone; Anna Golebiewska; Luciana R Gomes; Rodrigo Gomez; Rubén Gómez-Sánchez; Maria Catalina Gomez-Puerto; Raquel Gomez-Sintes; Qingqiu Gong; Felix M Goni; Javier González-Gallego; Tomas Gonzalez-Hernandez; Rosa A Gonzalez-Polo; Jose A Gonzalez-Reyes; Patricia González-Rodríguez; Ing Swie Goping; Marina S Gorbatyuk; Nikolai V Gorbunov; Kıvanç Görgülü; Roxana M Gorojod; Sharon M Gorski; Sandro Goruppi; Cecilia Gotor; 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; 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Siegfried Reipert; Rokeya Sultana Rekha; Hongmei Ren; Jun Ren; Weichao Ren; Tristan Renault; Giorgia Renga; Karen Reue; Kim Rewitz; Bruna Ribeiro de Andrade Ramos; S Amer Riazuddin; Teresa M Ribeiro-Rodrigues; Jean-Ehrland Ricci; Romeo Ricci; Victoria Riccio; Des R Richardson; Yasuko Rikihisa; Makarand V Risbud; Ruth M Risueño; Konstantinos Ritis; Salvatore Rizza; Rosario Rizzuto; Helen C Roberts; Luke D Roberts; Katherine J Robinson; Maria Carmela Roccheri; Stephane Rocchi; George G Rodney; Tiago Rodrigues; Vagner Ramon Rodrigues Silva; Amaia Rodriguez; Ruth Rodriguez-Barrueco; Nieves Rodriguez-Henche; Humberto Rodriguez-Rocha; Jeroen Roelofs; Robert S Rogers; Vladimir V Rogov; Ana I Rojo; Krzysztof Rolka; Vanina Romanello; Luigina Romani; Alessandra Romano; Patricia S Romano; David Romeo-Guitart; Luis C Romero; Montserrat Romero; Joseph C Roney; Christopher Rongo; Sante Roperto; Mathias T Rosenfeldt; Philip Rosenstiel; Anne G Rosenwald; Kevin A Roth; Lynn Roth; Steven Roth; Kasper M A Rouschop; 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Máté Varga; M Helena Vasconcelos; Somya Vats; Demetrios G Vavvas; Ignacio Vega-Naredo; Silvia Vega-Rubin-de-Celis; Guillermo Velasco; Ariadna P Velázquez; Tibor Vellai; Edo Vellenga; Francesca Velotti; Mireille Verdier; Panayotis Verginis; Isabelle Vergne; Paul Verkade; Manish Verma; Patrik Verstreken; Tim Vervliet; Jörg Vervoorts; Alexandre T Vessoni; Victor M Victor; Michel Vidal; Chiara Vidoni; Otilia V Vieira; Richard D Vierstra; Sonia Viganó; Helena Vihinen; Vinoy Vijayan; Miquel Vila; Marçal Vilar; José M Villalba; Antonio Villalobo; Beatriz Villarejo-Zori; Francesc Villarroya; Joan Villarroya; Olivier Vincent; Cecile Vindis; Christophe Viret; Maria Teresa Viscomi; Dora Visnjic; Ilio Vitale; David J Vocadlo; Olga V Voitsekhovskaja; Cinzia Volonté; Mattia Volta; Marta Vomero; Clarissa Von Haefen; Marc A Vooijs; Wolfgang Voos; Ljubica Vucicevic; Richard Wade-Martins; Satoshi Waguri; Kenrick A Waite; Shuji Wakatsuki; David W Walker; Mark J Walker; Simon A Walker; Jochen Walter; Francisco G Wandosell; 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: Daniel J Klionsky; Kotb Abdelmohsen; Akihisa Abe; Md Joynal Abedin; Hagai Abeliovich; Abraham Acevedo Arozena; Hiroaki Adachi; Christopher M Adams; Peter D Adams; Khosrow Adeli; Peter J Adhihetty; Sharon G Adler; Galila Agam; Rajesh Agarwal; Manish K Aghi; Maria Agnello; Patrizia Agostinis; Patricia V Aguilar; Julio Aguirre-Ghiso; Edoardo M Airoldi; Slimane Ait-Si-Ali; Takahiko Akematsu; Emmanuel T Akporiaye; Mohamed Al-Rubeai; Guillermo M Albaiceta; Chris Albanese; Diego Albani; Matthew L Albert; Jesus Aldudo; Hana Algül; Mehrdad Alirezaei; Iraide Alloza; Alexandru Almasan; Maylin Almonte-Beceril; Emad S Alnemri; Covadonga Alonso; Nihal Altan-Bonnet; Dario C Altieri; Silvia Alvarez; Lydia Alvarez-Erviti; Sandro Alves; Giuseppina Amadoro; Atsuo Amano; Consuelo Amantini; Santiago Ambrosio; Ivano Amelio; Amal O Amer; Mohamed Amessou; Angelika Amon; Zhenyi An; Frank A Anania; Stig U Andersen; Usha P Andley; Catherine K Andreadi; Nathalie Andrieu-Abadie; Alberto Anel; David K Ann; Shailendra Anoopkumar-Dukie; Manuela Antonioli; Hiroshi Aoki; Nadezda Apostolova; Saveria Aquila; Katia Aquilano; Koichi Araki; Eli Arama; Agustin Aranda; Jun Araya; Alexandre Arcaro; Esperanza Arias; Hirokazu Arimoto; Aileen R Ariosa; Jane L Armstrong; Thierry Arnould; Ivica Arsov; Katsuhiko Asanuma; Valerie Askanas; Eric Asselin; Ryuichiro Atarashi; Sally S Atherton; Julie D Atkin; Laura D Attardi; Patrick Auberger; Georg Auburger; Laure Aurelian; Riccardo Autelli; Laura Avagliano; Maria Laura Avantaggiati; Limor Avrahami; Suresh Awale; Neelam Azad; Tiziana Bachetti; Jonathan M Backer; Dong-Hun Bae; Jae-Sung Bae; Ok-Nam Bae; Soo Han Bae; Eric H Baehrecke; Seung-Hoon Baek; Stephen Baghdiguian; Agnieszka Bagniewska-Zadworna; Hua Bai; Jie Bai; Xue-Yuan Bai; Yannick Bailly; Kithiganahalli Narayanaswamy Balaji; Walter Balduini; Andrea Ballabio; Rena Balzan; Rajkumar Banerjee; Gábor Bánhegyi; Haijun Bao; Benoit Barbeau; Maria D Barrachina; Esther Barreiro; Bonnie Bartel; Alberto Bartolomé; Diane C Bassham; Maria Teresa Bassi; Robert C Bast; Alakananda Basu; Maria Teresa Batista; Henri Batoko; Maurizio Battino; Kyle Bauckman; Bradley L Baumgarner; K Ulrich Bayer; Rupert Beale; Jean-François Beaulieu; George R Beck; Christoph Becker; J David Beckham; Pierre-André Bédard; Patrick J Bednarski; Thomas J Begley; Christian Behl; Christian Behrends; Georg Mn Behrens; Kevin E Behrns; Eloy Bejarano; Amine Belaid; Francesca Belleudi; Giovanni Bénard; Guy Berchem; Daniele Bergamaschi; Matteo Bergami; Ben Berkhout; Laura Berliocchi; Amélie Bernard; Monique Bernard; Francesca Bernassola; Anne Bertolotti; Amanda S Bess; Sébastien Besteiro; Saverio Bettuzzi; Savita Bhalla; Shalmoli Bhattacharyya; Sujit K Bhutia; Caroline Biagosch; Michele Wolfe Bianchi; Martine Biard-Piechaczyk; Viktor Billes; Claudia Bincoletto; Baris Bingol; Sara W Bird; Marc Bitoun; Ivana Bjedov; Craig Blackstone; Lionel Blanc; Guillermo A Blanco; Heidi Kiil Blomhoff; Emilio Boada-Romero; Stefan Böckler; Marianne Boes; Kathleen Boesze-Battaglia; Lawrence H Boise; Alessandra Bolino; Andrea Boman; Paolo Bonaldo; Matteo Bordi; Jürgen Bosch; Luis M Botana; Joelle Botti; German Bou; Marina Bouché; Marion Bouchecareilh; Marie-Josée Boucher; Michael E Boulton; Sebastien G Bouret; Patricia Boya; Michaël Boyer-Guittaut; Peter V Bozhkov; Nathan Brady; Vania Mm Braga; Claudio Brancolini; Gerhard H Braus; José M Bravo-San Pedro; Lisa A Brennan; Emery H Bresnick; Patrick Brest; Dave Bridges; Marie-Agnès Bringer; Marisa Brini; Glauber C Brito; Bertha Brodin; Paul S Brookes; Eric J Brown; Karen Brown; Hal E Broxmeyer; Alain Bruhat; Patricia Chakur Brum; John H Brumell; Nicola Brunetti-Pierri; Robert J Bryson-Richardson; Shilpa Buch; Alastair M Buchan; Hikmet Budak; Dmitry V Bulavin; Scott J Bultman; Geert Bultynck; Vladimir Bumbasirevic; Yan Burelle; Robert E Burke; Margit Burmeister; Peter Bütikofer; Laura Caberlotto; Ken Cadwell; Monika Cahova; Dongsheng Cai; Jingjing Cai; Qian Cai; Sara Calatayud; Nadine Camougrand; Michelangelo Campanella; Grant R Campbell; Matthew Campbell; Silvia Campello; Robin Candau; Isabella Caniggia; Lavinia Cantoni; Lizhi Cao; Allan B Caplan; Michele Caraglia; Claudio Cardinali; Sandra Morais Cardoso; Jennifer S Carew; Laura A Carleton; Cathleen R Carlin; Silvia Carloni; Sven R Carlsson; Didac Carmona-Gutierrez; Leticia Am Carneiro; Oliana Carnevali; Serena Carra; Alice Carrier; Bernadette Carroll; Caty Casas; Josefina Casas; Giuliana Cassinelli; Perrine Castets; Susana Castro-Obregon; Gabriella Cavallini; Isabella Ceccherini; Francesco Cecconi; Arthur I Cederbaum; Valentín Ceña; Simone Cenci; Claudia Cerella; Davide Cervia; Silvia Cetrullo; Hassan Chaachouay; Han-Jung Chae; Andrei S Chagin; Chee-Yin Chai; Gopal Chakrabarti; Georgios Chamilos; Edmond Yw Chan; Matthew Tv Chan; Dhyan Chandra; Pallavi Chandra; Chih-Peng Chang; Raymond Chuen-Chung Chang; Ta Yuan Chang; John C Chatham; Saurabh Chatterjee; Santosh Chauhan; Yongsheng Che; Michael E Cheetham; Rajkumar Cheluvappa; Chun-Jung Chen; Gang Chen; Guang-Chao Chen; Guoqiang Chen; Hongzhuan Chen; Jeff W Chen; Jian-Kang Chen; Min Chen; Mingzhou Chen; Peiwen Chen; Qi Chen; Quan Chen; Shang-Der Chen; Si Chen; Steve S-L Chen; Wei Chen; Wei-Jung Chen; Wen Qiang Chen; Wenli Chen; Xiangmei Chen; Yau-Hung Chen; Ye-Guang Chen; Yin Chen; Yingyu Chen; Yongshun Chen; Yu-Jen Chen; Yue-Qin Chen; Yujie Chen; Zhen Chen; Zhong Chen; Alan Cheng; Christopher Hk Cheng; Hua Cheng; Heesun Cheong; Sara Cherry; Jason Chesney; Chun Hei Antonio Cheung; Eric Chevet; Hsiang Cheng Chi; Sung-Gil Chi; Fulvio Chiacchiera; Hui-Ling Chiang; Roberto Chiarelli; Mario Chiariello; Marcello Chieppa; Lih-Shen Chin; Mario Chiong; Gigi Nc Chiu; Dong-Hyung Cho; Ssang-Goo Cho; William C Cho; Yong-Yeon Cho; Young-Seok Cho; Augustine Mk Choi; Eui-Ju Choi; Eun-Kyoung Choi; Jayoung Choi; Mary E Choi; Seung-Il Choi; Tsui-Fen Chou; Salem Chouaib; Divaker Choubey; Vinay Choubey; Kuan-Chih Chow; Kamal Chowdhury; Charleen T Chu; Tsung-Hsien Chuang; Taehoon Chun; Hyewon Chung; Taijoon Chung; Yuen-Li Chung; Yong-Joon Chwae; Valentina Cianfanelli; Roberto Ciarcia; Iwona A Ciechomska; Maria Rosa Ciriolo; Mara Cirone; Sofie Claerhout; Michael J Clague; Joan Clària; Peter Gh Clarke; Robert Clarke; Emilio Clementi; Cédric Cleyrat; Miriam Cnop; Eliana M Coccia; Tiziana Cocco; Patrice Codogno; Jörn Coers; Ezra Ew Cohen; David Colecchia; Luisa Coletto; Núria S Coll; Emma Colucci-Guyon; Sergio Comincini; Maria Condello; Katherine L Cook; Graham H Coombs; Cynthia D Cooper; J Mark Cooper; Isabelle Coppens; Maria Tiziana Corasaniti; Marco Corazzari; Ramon Corbalan; Elisabeth Corcelle-Termeau; Mario D Cordero; Cristina Corral-Ramos; Olga Corti; Andrea Cossarizza; Paola Costelli; Safia Costes; Susan L Cotman; Ana Coto-Montes; Sandra Cottet; Eduardo Couve; Lori R Covey; L Ashley Cowart; Jeffery S Cox; Fraser P Coxon; Carolyn B Coyne; Mark S Cragg; Rolf J Craven; Tiziana Crepaldi; Jose L Crespo; Alfredo Criollo; Valeria Crippa; Maria Teresa Cruz; Ana Maria Cuervo; Jose M Cuezva; Taixing Cui; Pedro R Cutillas; Mark J Czaja; Maria F Czyzyk-Krzeska; Ruben K Dagda; Uta Dahmen; Chunsun Dai; Wenjie Dai; Yun Dai; Kevin N Dalby; Luisa Dalla Valle; Guillaume Dalmasso; Marcello D'Amelio; Markus Damme; Arlette Darfeuille-Michaud; Catherine Dargemont; Victor M Darley-Usmar; Srinivasan Dasarathy; Biplab Dasgupta; Srikanta Dash; Crispin R Dass; Hazel Marie Davey; Lester M Davids; David Dávila; Roger J Davis; Ted M Dawson; Valina L Dawson; Paula Daza; Jackie de Belleroche; Paul de Figueiredo; Regina Celia Bressan Queiroz de Figueiredo; José de la Fuente; Luisa De Martino; Antonella De Matteis; Guido Ry De Meyer; Angelo De Milito; Mauro De Santi; Wanderley de Souza; Vincenzo De Tata; Daniela De Zio; Jayanta Debnath; Reinhard Dechant; Jean-Paul Decuypere; Shane Deegan; Benjamin Dehay; Barbara Del Bello; Dominic P Del Re; Régis Delage-Mourroux; Lea Md Delbridge; Louise Deldicque; Elizabeth Delorme-Axford; Yizhen Deng; Joern Dengjel; Melanie Denizot; Paul Dent; Channing J Der; Vojo Deretic; Benoît Derrien; Eric Deutsch; Timothy P Devarenne; Rodney J Devenish; Sabrina Di Bartolomeo; Nicola Di Daniele; Fabio Di Domenico; Alessia Di Nardo; Simone Di Paola; Antonio Di Pietro; Livia Di Renzo; Aaron DiAntonio; Guillermo Díaz-Araya; Ines Díaz-Laviada; Maria T Diaz-Meco; Javier Diaz-Nido; Chad A Dickey; Robert C Dickson; Marc Diederich; Paul Digard; Ivan Dikic; Savithrama P Dinesh-Kumar; Chan Ding; Wen-Xing Ding; Zufeng Ding; Luciana Dini; Jörg Hw Distler; Abhinav Diwan; Mojgan Djavaheri-Mergny; Kostyantyn Dmytruk; Renwick Cj Dobson; Volker Doetsch; Karol Dokladny; Svetlana Dokudovskaya; Massimo Donadelli; X Charlie Dong; Xiaonan Dong; Zheng Dong; Terrence M Donohue; Kelly S Doran; Gabriella D'Orazi; Gerald W Dorn; Victor Dosenko; Sami Dridi; Liat Drucker; Jie Du; Li-Lin Du; Lihuan Du; André du Toit; Priyamvada Dua; Lei Duan; Pu Duann; Vikash Kumar Dubey; Michael R Duchen; Michel A Duchosal; Helene Duez; Isabelle Dugail; Verónica I Dumit; Mara C Duncan; Elaine A Dunlop; William A Dunn; Nicolas Dupont; Luc Dupuis; Raúl V Durán; Thomas M Durcan; Stéphane Duvezin-Caubet; Umamaheswar Duvvuri; Vinay Eapen; Darius Ebrahimi-Fakhari; Arnaud Echard; Leopold Eckhart; Charles L Edelstein; Aimee L Edinger; Ludwig Eichinger; Tobias Eisenberg; Avital Eisenberg-Lerner; N Tony Eissa; Wafik S El-Deiry; Victoria El-Khoury; Zvulun Elazar; Hagit Eldar-Finkelman; Chris Jh Elliott; Enzo Emanuele; Urban Emmenegger; Nikolai Engedal; Anna-Mart Engelbrecht; Simone Engelender; Jorrit M Enserink; Ralf Erdmann; Jekaterina Erenpreisa; Rajaraman Eri; Jason L Eriksen; Andreja Erman; Ricardo Escalante; Eeva-Liisa Eskelinen; Lucile Espert; Lorena Esteban-Martínez; Thomas J Evans; Mario Fabri; Gemma Fabrias; Cinzia Fabrizi; Antonio Facchiano; Nils J Færgeman; Alberto Faggioni; W Douglas Fairlie; Chunhai Fan; Daping Fan; Jie Fan; Shengyun Fang; Manolis Fanto; Alessandro Fanzani; Thomas Farkas; Mathias Faure; Francois B Favier; Howard Fearnhead; Massimo Federici; Erkang Fei; Tania C Felizardo; Hua Feng; Yibin Feng; Yuchen Feng; Thomas A Ferguson; Álvaro F Fernández; Maite G Fernandez-Barrena; Jose C Fernandez-Checa; Arsenio Fernández-López; Martin E Fernandez-Zapico; Olivier Feron; Elisabetta Ferraro; Carmen Veríssima Ferreira-Halder; Laszlo Fesus; Ralph Feuer; Fabienne C Fiesel; Eduardo C Filippi-Chiela; Giuseppe Filomeni; Gian Maria Fimia; John H Fingert; Steven Finkbeiner; Toren Finkel; Filomena Fiorito; Paul B Fisher; Marc Flajolet; Flavio Flamigni; Oliver Florey; Salvatore Florio; R Andres Floto; Marco Folini; Carlo Follo; Edward A Fon; Francesco Fornai; Franco Fortunato; Alessandro Fraldi; Rodrigo Franco; Arnaud Francois; Aurélie François; Lisa B Frankel; Iain Dc Fraser; Norbert Frey; Damien G Freyssenet; Christian Frezza; Scott L Friedman; Daniel E Frigo; Dongxu Fu; José M Fuentes; Juan Fueyo; Yoshio Fujitani; Yuuki Fujiwara; Mikihiro Fujiya; Mitsunori Fukuda; Simone Fulda; Carmela Fusco; Bozena Gabryel; Matthias Gaestel; Philippe Gailly; Malgorzata Gajewska; Sehamuddin Galadari; Gad Galili; Inmaculada Galindo; Maria F Galindo; Giovanna Galliciotti; Lorenzo Galluzzi; Luca Galluzzi; Vincent Galy; Noor Gammoh; Sam Gandy; Anand K Ganesan; Swamynathan Ganesan; Ian G Ganley; Monique Gannagé; Fen-Biao Gao; Feng Gao; Jian-Xin Gao; Lorena García Nannig; Eleonora García Véscovi; Marina Garcia-Macía; Carmen Garcia-Ruiz; Abhishek D Garg; Pramod Kumar Garg; Ricardo Gargini; Nils Christian Gassen; Damián Gatica; Evelina Gatti; Julie Gavard; Evripidis Gavathiotis; Liang Ge; Pengfei Ge; Shengfang Ge; Po-Wu Gean; Vania Gelmetti; Armando A Genazzani; Jiefei Geng; Pascal Genschik; Lisa Gerner; Jason E Gestwicki; David A Gewirtz; Saeid Ghavami; Eric Ghigo; Debabrata Ghosh; Anna Maria Giammarioli; Francesca Giampieri; Claudia Giampietri; Alexandra Giatromanolaki; Derrick J Gibbings; Lara Gibellini; Spencer B Gibson; Vanessa Ginet; Antonio Giordano; Flaviano Giorgini; Elisa Giovannetti; Stephen E Girardin; Suzana Gispert; Sandy Giuliano; Candece L Gladson; Alvaro Glavic; Martin Gleave; Nelly Godefroy; Robert M Gogal; Kuppan Gokulan; Gustavo H Goldman; Delia Goletti; Michael S Goligorsky; Aldrin V Gomes; Ligia C Gomes; Hernando Gomez; Candelaria Gomez-Manzano; Rubén Gómez-Sánchez; Dawit Ap Gonçalves; Ebru Goncu; Qingqiu Gong; Céline Gongora; Carlos B Gonzalez; Pedro Gonzalez-Alegre; Pilar Gonzalez-Cabo; Rosa Ana González-Polo; Ing Swie Goping; Carlos Gorbea; Nikolai V Gorbunov; Daphne R Goring; Adrienne M Gorman; Sharon M Gorski; Sandro Goruppi; Shino Goto-Yamada; Cecilia Gotor; Roberta A Gottlieb; Illana Gozes; Devrim Gozuacik; Yacine Graba; Martin Graef; Giovanna E Granato; Gary Dean Grant; Steven Grant; Giovanni Luca Gravina; Douglas R Green; Alexander Greenhough; Michael T Greenwood; Benedetto Grimaldi; Frédéric Gros; Charles Grose; Jean-Francois Groulx; Florian Gruber; Paolo Grumati; Tilman Grune; Jun-Lin Guan; Kun-Liang Guan; Barbara Guerra; Carlos Guillen; Kailash Gulshan; Jan Gunst; Chuanyong Guo; Lei Guo; Ming Guo; Wenjie Guo; Xu-Guang Guo; Andrea A Gust; Åsa B Gustafsson; Elaine Gutierrez; Maximiliano G Gutierrez; Ho-Shin Gwak; Albert Haas; James E Haber; Shinji Hadano; Monica Hagedorn; David R Hahn; Andrew J Halayko; Anne Hamacher-Brady; Kozo Hamada; Ahmed Hamai; Andrea Hamann; Maho Hamasaki; Isabelle Hamer; Qutayba Hamid; Ester M Hammond; Feng Han; Weidong Han; James T Handa; John A Hanover; Malene Hansen; Masaru Harada; Ljubica Harhaji-Trajkovic; J Wade Harper; Abdel Halim Harrath; Adrian L Harris; James Harris; Udo Hasler; Peter Hasselblatt; Kazuhisa Hasui; Robert G Hawley; Teresa S Hawley; Congcong He; Cynthia Y He; Fengtian He; Gu He; Rong-Rong He; Xian-Hui He; You-Wen He; Yu-Ying He; Joan K Heath; Marie-Josée Hébert; Robert A Heinzen; Gudmundur Vignir Helgason; Michael Hensel; Elizabeth P Henske; Chengtao Her; Paul K Herman; Agustín Hernández; Carlos Hernandez; Sonia Hernández-Tiedra; Claudio Hetz; P Robin Hiesinger; Katsumi Higaki; Sabine Hilfiker; Bradford G Hill; Joseph A Hill; William D Hill; Keisuke Hino; Daniel Hofius; Paul Hofman; Günter U Höglinger; Jörg Höhfeld; Marina K Holz; Yonggeun Hong; David A Hood; Jeroen Jm Hoozemans; Thorsten Hoppe; Chin Hsu; Chin-Yuan Hsu; Li-Chung Hsu; Dong Hu; Guochang Hu; Hong-Ming Hu; Hongbo Hu; Ming Chang Hu; Yu-Chen Hu; Zhuo-Wei Hu; Fang Hua; Ya Hua; Canhua Huang; Huey-Lan Huang; Kuo-How Huang; Kuo-Yang Huang; Shile Huang; Shiqian Huang; Wei-Pang Huang; Yi-Ran Huang; Yong Huang; Yunfei Huang; Tobias B Huber; Patricia Huebbe; Won-Ki Huh; Juha J Hulmi; Gang Min Hur; James H Hurley; Zvenyslava Husak; Sabah Na Hussain; Salik Hussain; Jung Jin Hwang; Seungmin Hwang; Thomas Is Hwang; Atsuhiro Ichihara; Yuzuru Imai; Carol Imbriano; Megumi Inomata; Takeshi Into; Valentina Iovane; Juan L Iovanna; Renato V Iozzo; Nancy Y Ip; Javier E Irazoqui; Pablo Iribarren; Yoshitaka Isaka; Aleksandra J Isakovic; Harry Ischiropoulos; Jeffrey S Isenberg; Mohammad Ishaq; Hiroyuki Ishida; Isao Ishii; Jane E Ishmael; Ciro Isidoro; Ken-Ichi Isobe; Erika Isono; Shohreh Issazadeh-Navikas; Koji Itahana; Eisuke Itakura; Andrei I Ivanov; Anand Krishnan V Iyer; José M Izquierdo; Yotaro Izumi; Valentina Izzo; Marja Jäättelä; Nadia Jaber; Daniel John Jackson; William T Jackson; Tony George Jacob; Thomas S Jacques; Chinnaswamy Jagannath; Ashish Jain; Nihar Ranjan Jana; Byoung Kuk Jang; Alkesh Jani; Bassam Janji; Paulo Roberto Jannig; Patric J Jansson; Steve Jean; Marina Jendrach; Ju-Hong Jeon; Niels Jessen; Eui-Bae Jeung; Kailiang Jia; Lijun Jia; Hong Jiang; Hongchi Jiang; Liwen Jiang; Teng Jiang; Xiaoyan Jiang; Xuejun Jiang; Xuejun Jiang; Ying Jiang; Yongjun Jiang; Alberto Jiménez; Cheng Jin; Hongchuan Jin; Lei Jin; Meiyan Jin; Shengkan Jin; Umesh Kumar Jinwal; Eun-Kyeong Jo; Terje Johansen; Daniel E Johnson; Gail Vw Johnson; James D Johnson; Eric Jonasch; Chris Jones; Leo Ab Joosten; Joaquin Jordan; Anna-Maria Joseph; Bertrand Joseph; Annie M Joubert; Dianwen Ju; Jingfang Ju; Hsueh-Fen Juan; Katrin Juenemann; Gábor Juhász; Hye Seung Jung; Jae U Jung; Yong-Keun Jung; Heinz Jungbluth; Matthew J Justice; Barry Jutten; Nadeem O Kaakoush; 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Jin Hyoung Kim; Kwang Woon Kim; Michael D Kim; Moon-Moo Kim; Peter K Kim; Seong Who Kim; Soo-Youl Kim; Yong-Sun Kim; Yonghyun Kim; Adi Kimchi; Alec C Kimmelman; Tomonori Kimura; Jason S King; Karla Kirkegaard; Vladimir Kirkin; Lorrie A Kirshenbaum; Shuji Kishi; Yasuo Kitajima; Katsuhiko Kitamoto; Yasushi Kitaoka; Kaio Kitazato; Rudolf A Kley; Walter T Klimecki; Michael Klinkenberg; Jochen Klucken; Helene Knævelsrud; Erwin Knecht; Laura Knuppertz; Jiunn-Liang Ko; Satoru Kobayashi; Jan C Koch; Christelle Koechlin-Ramonatxo; Ulrich Koenig; Young Ho Koh; Katja Köhler; Sepp D Kohlwein; Masato Koike; Masaaki Komatsu; Eiki Kominami; Dexin Kong; Hee Jeong Kong; Eumorphia G Konstantakou; Benjamin T Kopp; Tamas Korcsmaros; Laura Korhonen; Viktor I Korolchuk; Nadya V Koshkina; Yanjun Kou; Michael I Koukourakis; Constantinos Koumenis; Attila L Kovács; Tibor Kovács; Werner J Kovacs; Daisuke Koya; Claudine Kraft; Dimitri Krainc; Helmut Kramer; Tamara Kravic-Stevovic; Wilhelm Krek; Carole Kretz-Remy; Roswitha Krick; Malathi Krishnamurthy; Janos Kriston-Vizi; Guido Kroemer; Michael C Kruer; Rejko Kruger; Nicholas T Ktistakis; Kazuyuki Kuchitsu; Christian Kuhn; Addanki Pratap Kumar; Anuj Kumar; Ashok Kumar; Deepak Kumar; Dhiraj Kumar; Rakesh Kumar; Sharad Kumar; Mondira Kundu; Hsing-Jien Kung; Atsushi Kuno; Sheng-Han Kuo; Jeff Kuret; Tino Kurz; Terry Kwok; Taeg Kyu Kwon; Yong Tae Kwon; Irene Kyrmizi; Albert R La Spada; Frank Lafont; Tim Lahm; Aparna Lakkaraju; Truong Lam; Trond Lamark; Steve Lancel; Terry H Landowski; Darius J R Lane; Jon D Lane; Cinzia Lanzi; Pierre Lapaquette; Louis R Lapierre; Jocelyn Laporte; Johanna Laukkarinen; Gordon W Laurie; Sergio Lavandero; Lena Lavie; Matthew J LaVoie; Betty Yuen Kwan Law; Helen Ka-Wai Law; Kelsey B Law; Robert Layfield; Pedro A Lazo; Laurent Le Cam; Karine G Le Roch; Hervé Le Stunff; Vijittra Leardkamolkarn; Marc Lecuit; Byung-Hoon Lee; Che-Hsin Lee; Erinna F Lee; Gyun Min Lee; He-Jin Lee; Hsinyu Lee; Jae Keun Lee; Jongdae Lee; Ju-Hyun Lee; Jun Hee Lee; Michael Lee; Myung-Shik Lee; Patty J Lee; Sam W Lee; Seung-Jae Lee; Shiow-Ju Lee; Stella Y Lee; Sug Hyung Lee; Sung Sik Lee; Sung-Joon Lee; Sunhee Lee; Ying-Ray Lee; Yong J Lee; Young H Lee; Christiaan Leeuwenburgh; Sylvain Lefort; Renaud Legouis; Jinzhi Lei; Qun-Ying Lei; David A Leib; Gil Leibowitz; Istvan Lekli; Stéphane D Lemaire; John J Lemasters; Marius K Lemberg; Antoinette Lemoine; Shuilong Leng; Guido Lenz; Paola Lenzi; Lilach O Lerman; Daniele Lettieri Barbato; Julia I-Ju Leu; Hing Y Leung; Beth Levine; Patrick A Lewis; Frank Lezoualc'h; Chi Li; Faqiang Li; Feng-Jun Li; Jun Li; Ke Li; Lian Li; Min Li; Min Li; Qiang Li; Rui Li; Sheng Li; Wei Li; Wei Li; Xiaotao Li; Yumin Li; Jiqin Lian; Chengyu Liang; Qiangrong Liang; Yulin Liao; Joana Liberal; Pawel P Liberski; Pearl Lie; Andrew P Lieberman; Hyunjung Jade Lim; Kah-Leong Lim; Kyu Lim; Raquel T Lima; Chang-Shen Lin; Chiou-Feng Lin; Fang Lin; Fangming Lin; Fu-Cheng Lin; Kui Lin; Kwang-Huei Lin; Pei-Hui Lin; Tianwei Lin; Wan-Wan Lin; Yee-Shin Lin; Yong Lin; Rafael Linden; Dan Lindholm; Lisa M Lindqvist; Paul Lingor; Andreas Linkermann; Lance A Liotta; Marta M Lipinski; Vitor A Lira; Michael P Lisanti; Paloma B Liton; Bo Liu; Chong Liu; Chun-Feng Liu; Fei Liu; Hung-Jen Liu; Jianxun Liu; Jing-Jing Liu; Jing-Lan Liu; Ke Liu; Leyuan Liu; Liang Liu; Quentin Liu; Rong-Yu Liu; Shiming Liu; Shuwen Liu; Wei Liu; Xian-De Liu; Xiangguo Liu; Xiao-Hong Liu; Xinfeng Liu; Xu Liu; Xueqin Liu; Yang Liu; Yule Liu; Zexian Liu; Zhe Liu; Juan P Liuzzi; Gérard Lizard; Mila Ljujic; Irfan J Lodhi; Susan E Logue; Bal L Lokeshwar; Yun Chau Long; Sagar Lonial; Benjamin Loos; Carlos López-Otín; Cristina López-Vicario; Mar Lorente; Philip L Lorenzi; Péter Lõrincz; Marek Los; Michael T Lotze; Penny E Lovat; Binfeng Lu; Bo Lu; Jiahong Lu; Qing Lu; She-Min Lu; Shuyan Lu; Yingying Lu; Frédéric Luciano; Shirley Luckhart; John Milton Lucocq; Paula Ludovico; Aurelia Lugea; Nicholas W Lukacs; Julian J Lum; Anders H Lund; Honglin Luo; Jia Luo; Shouqing Luo; Claudio Luparello; Timothy Lyons; Jianjie Ma; Yi Ma; Yong Ma; Zhenyi Ma; Juliano Machado; Glaucia M Machado-Santelli; Fernando Macian; Gustavo C MacIntosh; Jeffrey P MacKeigan; Kay F Macleod; John D MacMicking; Lee Ann MacMillan-Crow; Frank Madeo; Muniswamy Madesh; Julio Madrigal-Matute; Akiko Maeda; Tatsuya Maeda; Gustavo Maegawa; Emilia Maellaro; Hannelore Maes; Marta Magariños; Kenneth Maiese; Tapas K Maiti; Luigi Maiuri; Maria Chiara Maiuri; Carl G Maki; Roland Malli; Walter Malorni; Alina Maloyan; Fathia Mami-Chouaib; Na Man; Joseph D Mancias; Eva-Maria Mandelkow; Michael A Mandell; Angelo A Manfredi; Serge N Manié; Claudia Manzoni; Kai Mao; Zixu Mao; Zong-Wan Mao; Philippe Marambaud; Anna Maria Marconi; Zvonimir Marelja; Gabriella Marfe; Marta Margeta; Eva Margittai; Muriel Mari; Francesca V Mariani; Concepcio Marin; Sara Marinelli; Guillermo Mariño; Ivanka Markovic; Rebecca Marquez; Alberto M Martelli; Sascha Martens; Katie R Martin; Seamus J Martin; Shaun Martin; Miguel A Martin-Acebes; Paloma Martín-Sanz; Camille Martinand-Mari; Wim Martinet; Jennifer Martinez; Nuria Martinez-Lopez; Ubaldo Martinez-Outschoorn; Moisés Martínez-Velázquez; Marta Martinez-Vicente; Waleska Kerllen Martins; Hirosato Mashima; James A Mastrianni; Giuseppe Matarese; Paola Matarrese; Roberto Mateo; Satoaki Matoba; Naomichi Matsumoto; Takehiko Matsushita; Akira Matsuura; Takeshi Matsuzawa; Mark P Mattson; Soledad Matus; Norma Maugeri; Caroline Mauvezin; Andreas Mayer; Dusica Maysinger; Guillermo D Mazzolini; Mary Kate McBrayer; Kimberly McCall; Craig McCormick; Gerald M McInerney; Skye C McIver; Sharon McKenna; John J McMahon; Iain A McNeish; Fatima Mechta-Grigoriou; Jan Paul Medema; Diego L Medina; Klara Megyeri; Maryam Mehrpour; Jawahar L Mehta; Yide Mei; Ute-Christiane Meier; Alfred J Meijer; Alicia Meléndez; Gerry Melino; Sonia Melino; Edesio Jose Tenorio de Melo; Maria A Mena; Marc D Meneghini; Javier A Menendez; Regina Menezes; Liesu Meng; Ling-Hua Meng; Songshu Meng; Rossella Menghini; A Sue Menko; Rubem Fs Menna-Barreto; Manoj B Menon; Marco A Meraz-Ríos; Giuseppe Merla; Luciano Merlini; Angelica M Merlot; Andreas Meryk; Stefania Meschini; Joel N Meyer; Man-Tian Mi; Chao-Yu Miao; Lucia Micale; Simon Michaeli; Carine Michiels; Anna Rita Migliaccio; Anastasia Susie Mihailidou; Dalibor Mijaljica; Katsuhiko Mikoshiba; Enrico Milan; Leonor Miller-Fleming; Gordon B Mills; Ian G Mills; Georgia Minakaki; Berge A Minassian; Xiu-Fen Ming; Farida Minibayeva; Elena A Minina; Justine D Mintern; Saverio Minucci; Antonio Miranda-Vizuete; Claire H Mitchell; Shigeki Miyamoto; Keisuke Miyazawa; Noboru Mizushima; Katarzyna Mnich; Baharia Mograbi; Simin Mohseni; Luis Ferreira Moita; Marco Molinari; Maurizio Molinari; Andreas Buch Møller; Bertrand Mollereau; Faustino Mollinedo; Marco Mongillo; Martha M Monick; Serena Montagnaro; Craig Montell; Darren J Moore; Michael N Moore; Rodrigo Mora-Rodriguez; Paula I Moreira; Etienne Morel; Maria Beatrice Morelli; Sandra Moreno; 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