Literature DB >> 31225455

p38β MAPK mediates ULK1-dependent induction of autophagy in skeletal muscle of tumor-bearing mice.

Zhelong Liu^1,2, Ka Wai Thomas Sin¹, Hui Ding^1,3, HoangAnh Amy Doan¹, Song Gao¹, Hongyu Miao⁴, Yahui Wei¹, Yiman Wang¹, Guohua Zhang¹, Yi-Ping Li¹.

Abstract

Muscle wasting is the key manifestation of cancer-associated cachexia, a lethal metabolic disorder seen in over 50% of cancer patients. Autophagy is activated in cachectic muscle of cancer hosts along with the ubiquitin-proteasome pathway (UPP), contributing to accelerated protein degradation and muscle wasting. However, established signaling mechanism that activates autophagy in response to fasting or denervation does not seem to mediate cancer-provoked autophagy in skeletal myocytes. Here, we show that p38β MAPK mediates autophagy activation in cachectic muscle of tumor-bearing mice via novel mechanisms. Complementary genetic and pharmacological manipulations reveal that activation of p38β MAPK, but not p38α MAPK, is necessary and sufficient for Lewis lung carcinoma (LLC)-induced autophagy activation in skeletal muscle cells. Particularly, muscle-specific knockout of p38β MAPK abrogates LLC tumor-induced activation of autophagy and UPP, sparing tumor-bearing mice from muscle wasting. Mechanistically, p38β MAPK-mediated activation of transcription factor C/EBPβ is required for LLC-induced autophagy activation, and upregulation of autophagy-related genes LC3b and Gabarapl1. Surprisingly, ULK1 activation (phosphorylation at S555) by cancer requires p38β MAPK, rather than AMPK. Activated ULK1 forms a complex with p38β MAPK in myocytes, which is markedly increased by a tumor burden. Overexpression of a constitutively active p38Tbeta; MAPK in HEK293 cells increases phosphorylation at S555 and other amino acid residues of ULK1, but not several of AMPK-mediated sites. Finally, ULK1 activation is abrogated in tumor-bearing mice with muscle-specific knockout of p38β MAPK. Thus, p38β MAPK appears a key mediator of cancer-provoked autophagy activation, and a therapeutic target of cancer-induced muscle wasting.

Entities: CellLine Chemical Disease Gene Species

Keywords: C/EBPβ; Gabarapl1; LC3b; ULK1; cachexia; muscle wasting

Year: 2018 PMID： 31225455 PMCID： PMC6551802 DOI： 10.15698/cst2018.11.163

Source DB: PubMed Journal: Cell Stress ISSN： 2523-0204

INTRODUCTION

Cancer has been increasingly recognized as a systemic disorder that stresses multiple organs independent of its location. At least 50% of cancer patients experience cachexia, a systemic wasting syndrome manifested as weight loss, inflammation, insulin resistance, and increased muscle protein breakdown. Progressive loss of muscle mass (muscle wasting) contributes significantly to cancer-associated morbidity and mortality 12. However, the etiology of cancer cachexia is not well defined and there is no FDA-approved treatment for this lethal disorder. There has been a general consensus that accelerated muscle protein degradation is a major cause of cachexia-associated muscle mass loss. It has been well-established that the ubiquitin proteasome pathway (UPP) plays an important role in cancer-induced muscle wasting by degrading myofibrillar proteins 345. More recent evidence indicates that cancer also induces autophagy activation in the cachectic muscle of tumor-bearing mice 6789 and cancer patients 101112. Autophagy targets cytoplasmic constituents including ubiquitinated protein aggregates and organelles for degradation by lysosomes 1314. Autophagy inhibition blocks muscle protein degradation induced by the activation of Toll-like receptor 4 (TLR4) 15, a plasma membrane receptor that is activated by danger-associated molecular patterns (DAMPs)16 and mediates cancer-induced muscle wasting 4917. Thus, cancer-provoked autophagy activation is considered a therapeutic target of cancer-induced muscle wasting. However, the intramuscular signaling pathways that mediate cancer-induced activation of autophagy remain poorly understood. Elucidating and thereby targeting the cellular signaling pathways that mediate cancer-induced activation of autophagy could allow intervention of cancer-induced muscle wasting. The Akt-FoxO signaling pathway inversely mediates the activity of both autophagy and UPP in muscle in response to such catabolic stimuli as fasting or denervation 1819. However, Akt is activated in cachectic muscle of tumor-bearing mice 2021 and cancer patients 1112, which inhibits FoxOs by promoting their translocation out of nuclei 22. Thus, the Akt-FoxO signaling pathway does not appear to mediate cancer-induced muscle catabolism that is due largely to systemic inflammation. On the other hand, we observed previously that inflammation activated-p38 MAPK mediates both the autophagy and UPP activation in skeletal muscle in response to TLR4 activation by lipopolysaccharide 15. Other inflammatory mediators implicated in cancer cachexia also activate p38 MAPK including oxidative stress 23, TNFα 24, IL-6 25, IL-1 26, TWEAK 27, activin A/myostatin 28 as well as extracellular Hsp70 and Hsp90 4, while promoting autophagy and/or UPP-mediated muscle protein loss. However, it is unknown which of the three p38 MAPK isoforms that are expressed in skeletal muscle ((, (, and () mediates cancer-induced autophagy activation. More importantly, how p38 MAPK activates autophagy is unknown. In the present study, we demonstrate that activation of the p38β MAPK isoform is necessary and sufficient for autophagy activation in skeletal muscle in a mouse model of cancer cachexia, and that deletion of p38β MAPK in skeletal muscle abrogates muscle wasting by attenuating muscle protein degradation mediated by autophagy as well as UPP. Mechanistically, p38Tbeta; MAPK mediates cancer-provoked autophagy activation by upregulating Atg8 orthologues LC3b and Gabarapl1 as well as by activating ULK1. These data support p38β MAPK as a key mediator and therapeutic target of cancer-associated muscle wasting.

RESULTS

LLC induces autophagy activation in skeletal muscle cells through p38β MAPK

We previously showed that LLC induces an increase in autophagy flux and autophagosome formation in cultured C2C12 myotubes as well as mouse muscle 9. In the present study, we further investigated whether LLC induces autophagy activation in skeletal muscle cells through p38 MAPK by monitoring the autophagy marker LC3-II. By pretreating C2C12 myotubes, which respond to cancer cell-conditioned media in a similar manner as primary myotubes 4, with a p38α/β MAPK inhibitor SB202190, we observed that the induction of autophagy by LLC cell-conditioned medium (LCM) required p38 MAPK activation (Figure 1A). In addition, systemic administration of SB202190 to LLC tumor-bearing mice inhibited autophagy activation in cachectic muscle (Figure 1B). These results suggest that LLC induces autophagy activation in skeletal muscle through the activation of p38α and/or p38β MAPK.

FIGURE 1: p38β MAPK activation is necessary and sufficient for autophagy activation by tumor in skeletal muscle cells.

(A) Inhibition of p38 MAPK attenuates LLC-conditioned medium (LCM)-induced autophagy activation in C2C12 myotubes. C2C12 myotubes were pretreated with SB202190 (SB, 10 (M) or vehicle (0.1% DMSO) for 30 min prior to treatment with LCM or control medium (NL20) for 8 h. Autophagy activation was evaluated by Western blotting analysis of LC3 in cell lysate. (B) Inhibition of p38 MAPK attenuates autophagy activation in skeletal muscle of LLC tumor-bearing mice. In 7 days of LLC implant to mice, SB202190 was i.p. injected (5 mg/kg) daily with DMSO (50%) as vehicle control for 14 days. Lysate of TA collected on 21 days of LLC implant was analyzed by Western blotting for LC3 (samples from 3 mice per group were loaded on each gel). (C) LCM-induced autophagy activation in myotubes is dependent on p38β MAPK. C2C12 myoblasts were transfected with control, p38α MAPK or p38β MAPK-specific siRNA. After differentiation, myotubes were treated with LCM or control medium for 8 h. Autophagy activation was evaluated by Western blotting analysis of LC3. (D) Expression of constitutively active p38β MAPK stimulates autophagy flux in C2C12 myotubes. Plasmids encoding a constitutively active mutant of p38α MAPK or p38β MAPK with the HA tag were transfected into C2C12 myoblasts, with empty vector as control. After differentiation, myotubes were treated with chloroquine (CQ, 20 (M) for 8 h. LC3, p62 and expression of the p38 MAPK mutants were monitored by Western blotting. (E) Constitutively active p38β MAPK activates autophagy in mouse muscle. Plasmids encoding the constitutively active mutant of p38α MAPK or p38β MAPK fused with the HA tag were transfected into the TA of mice. Empty vector was transfected into the contralateral TA. On day 14 expression of the p38 MAPK mutants and autophagy activation was analyzed by Western blotting (data from two mice per group are shown). Data were analyzed by one way ANOVA. * denotes a difference between bracketed groups or from controls (p < 0.05). (F) Constitutively active p38β MAPK stimulates autophagosome formation in mouse muscle. A plasmid encoding GFP-LC3 was transfected into mouse TA muscle, and co-transfected with the plasmid encoding the constitutively active mutant of p38α MAPK or p38β MAPK in the contralateral TA. In 7 days, TA muscle was collected. Frozen sections were prepared and stained with DAPI. Autophagosome formation was evaluated by confocal microscopy. Bars represent 50 μm. To identify the isoform of p38 MAPK that mediated LLC induction of autophagy, we utilized siRNA-mediated gene silencing and observed that the loss of p38β MAPK, but not p38α MAPK, abolished LCM-induced autophagy activation (Figure 1C). To examine whether activated p38β MAPK actually stimulated autophagy flux, a constitutively active mutant of p38α MAPK or p38β MAPK 29 was expressed in myotubes. Only the active p38β MAPK increased the LC3-II level. In addition, treatment of myotubes with lysosome inhibitor chloroquine (CQ) further increased LC3-II in active p38β MAPK-expressing myotubes. Further, expression of active p38β MAPK resulted in a loss in the autophagy-selective target p62, and CQ treatment abrogated this effect (Figure 1D). These results indicate that p38β MAPK activation stimulated autophagy flux. Similarly, LC3-II was specifically increased by the overexpressed active mutant of p38β MAPK in the muscle (TA) of tumor-free mice (Figure 1E). Furthermore, co-transfection of GFP-LC3 with active p38β MAPK, but not active p38α MAPK, in mouse muscle resulted in increased autophagosome formation as indicated by the formation of GFP-LC3-incorporated puncta (Figure 1F). These data provided evidence that p38β MAPK activation is necessary and sufficient for autophagy activation in skeletal muscle cells by a tumor burden.

LLC induces muscle wasting through p38β MAPK-mediated activation of autophagy and UPP

Next, we investigated whether LLC-induced activation of autophagy and muscle wasting are attenuated in the muscle of mice with muscle-specific knockout of p38β MAPK (p38β MKO) 30. It was previously shown that the muscle phenotype was not altered by deleting the p38β gene 283031. We observed that p38β MKO mice were resistant to LLC-induced autophagy activation as measured by LC3-II and p62 levels (Figure 2A). In addition, p38β MKO mice were resistant to LLC-stimulated UPP activity as monitored by the levels of atrogin1, UBR2 and myofibrillar protein myosin heavy chain (MHC) (Figure 2B). Consequently, p38β MKO mice were spared from LLC-induced muscle wasting without altering tumor growth as measured by tumor weight, body and muscle weight, muscle proteolysis (tyrosine release), muscle strength (grip strength, Figure 2C) and myofiber cross-sectional area (Figure 2D). Thus, LLC induces muscle wasting through p38β MAPK-mediated activation of both autophagy and UPP.

FIGURE 2: Muscle-specific knockout of p38β MAPK abrogates activation of autophagy, UPP and muscle wasting in tumor-bearing mice.

Mice with muscle-specific knockout of p38β MAPK and control mice (p38β MAPKf/f) were implanted with LLC cells. In 21 days, mice were euthanized for analysis of muscle wasting. Lysate of TA collected from the mice was analyzed by Western blotting for LC3 and p62 to evaluate autophagy activity (A) and UBR2, atrogin1 and MHC to evaluate UPP activity (B). Muscle wasting in the mice was analyzed by examining tumor weight, body and muscle weight, tyrosine release and grip strength (C). Muscle mass was measured as muscle fiber cross sectional area (D). Data in A to C were analyzed by one way ANOVA. Data in D were analyzed by Chi-square analysis. * denotes a difference (p < 0.05).

p38β MAPK-mediated C/EBPβ activation is critical to LLC-induced autophagy activation

We previously showed that p38β MAPK mediates LLC-induced upregulation of atrogin1 29 and UBR2 32 through the activation of C/EBPβ-binding to a cis-element in their 5’-promoter by phosphorylating the Thr-188 residue of C/EBPβ 29, and that LLC-induced muscle wasting is abrogated in C/EBPβ knockout mice 21. We therefore investigated whether the p38β MAPK → C/EBPβ signaling pathway also mediates LLC activation of autophagy. We observed that LLC-induced activation of C/EBPβ was blocked in the muscle of p38β MKO mice (Figure 3A), confirming in vivo that p38β MAPK mediates LLC-induced activation of C/EBPβ. To investigate whether C/EBPβ is critical to LLC-induced autophagy activation, we treated C/EBPβ-deficient C2C12 myotubes with LCM, and observed a dependence of LCM-induced autophagy activation on C/EBPβ (Figure 3B). Further, we observed that LLC-induced autophagy activation was abrogated in the muscle of C/EBPβ knockout mice (Figure 3C). Thus, p38β MAPK-mediated activation of C/EBPβ is critical to LLC-induced autophagy activation.

FIGURE 3: The p38β MAPK → C/EBPβ signaling pathway mediates autophagy activation by tumor in skeletal muscle cells.

(A) C/EBPβ activation in skeletal muscle of LLC tumor-bearing mice is dependent on p38β MAPK. Lysate of TA collected from p38β MAPKf/f and p38β MAPK muscle-specific knockout mice on day 21 of LLC implant was analyzed by Western blotting for C/EBPβ activation (phosphorylation of Thr-188). (B) C/EBPβ is critical to LCM-induced autophagy activation in myotubes. C2C12 myoblasts transfected with control or C/EBPβ-specific siRNA were treated with LCM or control medium for 8 h. C/EBPβ and LC3 were analyzed by Western blotting. (C) Autophagy activation in skeletal muscle of LLC tumor-bearing mice is dependent on C/EBPβ. Lysate of TA collected from wild type and C/EBPβ knockout mice on day 21 of LLC implant was analyzed by Western blotting for LC3.

p38β MAPK → C/EBPβ signaling mediates upregulation of specific autophagy-related genes

To understand how C/EBPβ mediates LLC-induced autophagy activation, we searched a data base (http://tfbind.hgc.jpfor potential C/EBPβ-binding sites in the 5’-promoter regions of autophagy-related genes and identified multiple sites within -1 kilo-bases in five important autophagy related genes (Figure 4A). By analyzing mRNA levels of these genes in the muscle of LLC tumor-bearing wild type and C/EBPβ knockout mice, we found that mRNA of LC3b and Gabarapl1, two Atg8 orthologues, were upregulated by LLC in a C/EBPβ-dependent manner (Figure 4B). Corroborative data were obtained in C2C12 myotubes where LCM treatment upregulated the two genes in a C/EBPβ-dependent manner (Figure 4C). To determine whether LLC stimulates C/EBPβ binding to the two gene promoters, we performed the chromatin immunoprecipitation (ChIP) assay and observed that LCM treatment of C2C12 myotubes stimulated C/EBPβ binding to multiple sites in the LC3b and Gabarapl1 promoter (Figure 4D). These data suggest that C/EBPβ upregulates the two Atg8 orthologues in muscle cells in response to a tumor burden.

FIGURE 4. C/EBPβ mediates tumor induction of autophagy-related genes in skeletal muscle cells.

(A) Potential C/EBPβ-binding cites are identified in autophagy-related genes. Data base search identified multiple potential biding sites of C/EBPβ in the 5’ promoter region of listed autophagy-related genes. (B) LC3b and Gabarapl1 are upregulated in skeletal muscle of LLC tumor-bearing mice in a C/EBPβ-dependent manner. Total RNA was extracted from the TA of wild type and C/EBPβ knockout mice implanted with LLC cells for 21 days, and analyzed for the mRNA of above identified autophagy-related genes by real-time PCR. (C) LC3b and Gabarapl1 are upregulated in LCM-treated myotubes in a C/EBPβ-dependent manner. Total RNA was extracted from C2C12 myotubes transfected with C/EBPβ-specific or control siRNA. The mRNA of C/EBPβ, LC3b and Gabarapl1 was determined by real-time PCR. Data from panel B and C were analyzed by one way ANOVA. * denotes a difference (p < 0.05). (D) LCM activates C/EBPβ binding to the LC3b and Gabarapl1 promoters in myotubes. C/EBPβ binding to the LC3b and Gabarapl1 promoters in C2C12 myotubes treated with LCM or the control NL20 cell-conditioned medium (NCM) was analyzed by the ChIP assay. Pre-immune IgG was used as control for C/EBPβ-specific antibody. To verify whether p38β MAPK is required for C/EBPβ-mediated upregulation of LC3b and Gabarapl1, we observed that the upregulation of these genes in LCM-treated myotubes was inhibited by SB202190 (Figure 5A). Further, upregulation of these genes in skeletal muscle was abrogated in LLC tumor-bearing p38β MKO mice (Figure 5B). These data confirm that LLC upregulates LC3b and Gabarapl1 through the p38β MAPK ( C/EBPβ signaling pathway.

FIGURE 5: p38β MAPK is required for upregulation of C/EBPβ-responsive autophagy-related genes in cachectic muscle of tumor-bearing mice.

(A) Inhibition of p38 MAPK attenuates LC3b and Gabarapl1 upregulation in cachectic muscle of LLC tumor-bearing mice. On day 7 of LLC cells implant to mice, SB202190 was i.p. injected (5 mg/kg) daily with DMSO (50%) as vehicle control. Lysate of TA collected on day 21 was analyzed by qPCR for LC3b and Gabarapl1 mRNA levels. (B) LC3b and Gabarapl1 upregulation in the muscle of LLC tumor-bearing mice is dependent on p38β MAPK. Mice with muscle-specific knockout of p38β MAPK (p38β MAPK MKO) or control mice (p38β MAPKf/f) were implanted with LLC cells. On day 21, total RNA was extracted from TA of the mice and analyzed by qPCR for LC3b and Gabarapl1 mRNA levels. Data were analyzed by one way ANOVA. * denotes a difference (p < 0.05).

LLC induces ULK1 activation in skeletal muscle through p38β MAPK

Both LC3b and Gabarapl1 are members of the ATG8 family that are essential for autophagosome formation 33. On the other hand, ATG8 family members must be activated by the ULK1 complex post-translationally to initiate the lipidation process required for autophagsome formation 34. Therefore, we examined whether LLC induced ULK1 activation in skeletal muscle cells. LCM treatment of C2C12 myotubes for 1 h increased ULK1 phosphorylation on Ser-555 (pS555-ULK1, Figure 6A). Phosphorylation of ULK1 on this serine residue is known to activate ULK1 by AMP-activated protein kinase (AMPK) upon nutrient deprivation 3536. LCM was shown previously to induce mTOR inhibition and AMPK activation in C2C12 myotubes 37. To examine the involvement of AMPK in LCM-induced activation of ULK1, we pretreated myotubes with the AMPK inhibitor Compound C 38. To our surprise, Compound C did not alter LCM-induced ULK1 phosphorylation on Ser-555, although it did inhibit AMPK activation as measured by the phosphorylation state of its Thr-172 residue. However, pretreatment with p38 MAPK inhibitor SB202190 attenuated LCM-induced Ser-555 phosphorylation of ULK-1, without affecting LCM-induced Thr-172 phosphorylation of AMPK (Figure 6A). These data suggest that p38 MAPK, rather than AMPK, is critical to LCM-induced activation of ULK1. We then investigated whether p38 MAPK interacted with ULK1 by performing immunoprecipitation of p38 MAPK from myotube lysate. We observed co-precipitation of pS555-ULK1 with p38 MAPK in control myotubes, and that the level of co-precipitated pS555-ULK1 dramatically increased in LCM-treated myotubes (Figure 6B), suggesting that p38 MAPK does interact with ULK1 resulting in phosphorylation of its Ser-555 residue in myocytes, and this activity is stimulated upon p38 MAPK activation by a tumor burden. To identify the p38 MAPK isoform responsible for LCM-stimulated ULK1 phosphorylation on Ser-555, we performed siRNA-mediated gene silencing in myotubes and observed that p38β MAPK, but not p38α MAPK, was required for this reaction (Figure 6C). To verify that activation of p38β MAPK is sufficient to phosphorylate ULK1, FLAG-tagged ULK1 was co-expressed with constitutively active p38β MAPK in HEK293T cells. Mass spectrometry analysis of FLAG-ULK1 isolated from cell lysate revealed multiple phosphorylated amino acid residues including Ser-555 (Supplementary Table 1). However, these sites did not include a number of known AMPK-mediated phosphorylation sites in ULK1 such as Ser-317, Ser-467, Ser-637 and Ser-777 3639. In combination, the above data support that p38β MAPK stimulates ULK1 activity upon activation by cancer independent of AMPK in the cellular environment. Finally, we confirmed that Ser-555 phosphorylation of ULK1 increased in the muscle of LLC tumor-bearing p38βf/f mice but not in that of muscle-specific p38β MAPK knockout mice. On the other hand, LLC-induced AMPK activation was not altered in p38β MAPK-deficient muscle (Figure 6E). Therefore, we conclude that p38β MAPK, rather than AMPK, mediates LLC-induced autophagosome formation by activating ULK1 in addition to upregulating LC3b and Gabarapl1.

FIGURE 6: p38β MAPK activates ULK1 in skeletal muscle cells in response to tumor.

(A) LCM stimulates ULK1 phosphorylation on Ser-555 in myotubes through p38 MAPK. C2C12 myotubes were pretreated with DMSO (0.1%, vehicle), compound C (CC, 10 (M) or SB202190 (SB, 10 (M) for 30 min, and then treated with LCM for 1 h. ULK1 phosphorylation state on Ser-555 and AMPK phosphorylation on Thr-172 in cell lysate were analyzed by Western blotting. (B) LCM stimulates p38 MAPK interaction with ULK1 in myotubes. C2C12 myotubes were treated with LCM for 1 h. Cell lysate was subjected to immunoprecipitation with pre-immune IgG or p38 MAPK-specific antibody. Precipitate was analyzed by Western blotting for p38 MAPK and pSer-555 ULK1. (C) LCM stimulation of ULK1 phosphorylation on Ser-555 in myotubes is mediated by p38β MAPK specifically. C2C12 myoblasts were transfected with control, p38β MAPK or p38β MAPK-specific siRNA. After differentiation for 96 h, myotubes were treated with LCM or control medium for 1 h. Knockdown of p38 MAPKs and phosphorylation of ULK1 on Ser-555 were analyzed by Western blotting. (D) p38β MAPK is required for ULK1 activation in cachectic muscle of LLC tumor-bearing mice. Mice with muscle-specific knockout of p38β MAPK and control mice were implanted with LLC cells. Lysate of TA collected from these mice on day 21 was analyzed by Western blotting for ULK1 phosphorylation on Ser-555 and AMPK phosphorylation on Thr-172. Data were analyzed by one way AVOVA. * denotes a difference (p < 0.05).

DISCUSSION

The current study identifies p38β MAPK as a key mediator of cancer-induced autophagy activation in skeletal muscle, through activating ULK1 as well as upregulating C/EBPβ-controlled LC3b and Gabarapl1 genes. Importantly, we were able to abrogate cancer-induced muscle wasting by deleting p38β MAPK in skeletal muscle to prevent muscle protein degradation mediated by autophagy as well as UPP. These findings suggest that p38β MAPK is a key mediator and a therapeutic target of cancer-induced muscle wasting. We show that p38β MAPK upregulates LC3b and Gabarapl1 through activating C/EBPβ. The LC3 and Gabarapl family of proteins are mammalian orthologues of ATG8, a yeast autophagy-related protein involved in the formation of autophagosomes 33. Increased expression of LC3/Gabaraple and activation of autophagy have been observed in cachectic muscle of cancer patients 101112. In various types of cells, increased expression of LC3/Gabarapl are often associated with autophagy activation 4041. As the substrates of ULK1-mediated lipidation process that is critical for autophagosome formation 34, increased expression of LC3/Gabarapl is likely to facilitate autophagosome formation. On the other hand, the possibility exists that C/EBPTbeta; may regulate additional autophagy-related genes that are rate-limiting for autophagosome formation. Autophagy is activated by nutritional deprivation through AMPK-mediated phosphorylation of ULK1 on multiple sites including Ser-555 in various cell types 3536. In skeletal muscle, autophagy is also activated by the inactivation of Akt that inversely regulates FoxO3-mediated upregulation of autophagy-related gene expression in response to denervation or starvation 1842, or by AMPK-mediated activation of FoxO3 in response to C26 colon adenocarcinoma 43. We previously showed that LLC activates Akt and inactivates FoxO1/3 in muscle cells, while activating p38 MAPK concomitantly 21. In the present study we show that despite AMPK activation by LLC in skeletal muscle, AMPK does not mediate in ULK1 activation LLC tumor-bearing mice. On the contrary, autophagy activation in skeletal muscle by LLC requires p38β MAPK-mediated activation of ULK1. Thus, tumor activates autophagy in skeletal muscle through a signaling mechanism distinct from that in nutritional deprivation. It is well-established that in skeletal muscle p38 MAPK is activated by various inflammatory mediators implicated in cancer cachexia including various cytokines 2425262728, reactive oxygen species (ROS)23 and extracellular vesicle-associated Hsp70 and Hsp90 4. Of the three members of p38 MAPK family expressed in skeletal muscle, p38α MAPK is responsible for most of the known roles of p38 MAPK including mediating inflammation 4445 and promoting myogenesis 4647. p38γ MAPK regulates the expansion of myogenic precursor cells 48, endurance exercise-induced mitochondrial biogenesis and angiogenesis 30, as well as glucose uptake 49. On the other hand, p38β MAPK has few known functions. Utilizing genetic manipulations including the p38β MAPK muscle specific knockout mice 30 in addition to pharmacological inhibition of p38α/β MAPK (due to the lack of p38β MAPK-specific inhibitors), the current study demonstrated for the first time that p38β MAPK is essential to autophagy activation during muscle wasting induced by LLC. The current study also demonstrated for the first time in vivo that p38β MAPK is essential to UPP activation and muscle wasting induced by cancer. Therefore, developing p38β MAPK-specific pharmacological inhibitors would be highly desirable for the intervention of cancer cachexia. Our findings on the role of p38β MAPK in autophagy activation may have significance beyond skeletal muscle cells. For example, p38 MAPK mediates various stress-induced autophagy activation in a variety of cells 5051525354. Particularly, in response to TLR4 activation, p38 MAPK mediates autophagy activation associated with innate immunity 55, which is similar to cancer-induced muscle wasting 4917. However, which p38 MAPK isoform and how it activates autophagy in those processes are unknown. It is possible that a similar mechanism as we observed in skeletal muscle cells exists in other types of cells to mediate autophagy activation in response to inflammatory stresses. Taken together, our findings reveal that p38β MAPK mediates cancer-induced autophagy in skeletal muscle through novel transcriptional as well as post-translational mechanisms. In addition, our findings suggest that cancer-induced muscle wasting can be ameliorated by targeting a single signaling molecule in skeletal muscle, p38β MAPK.

MATERIALS AND METHODS

Myogenic cell culture

Murine C2C12 myoblasts (American Type Culture Collection) were cultured in growth medium (DMEM supplemented with 10% fetal bovine serum) at 37(C with 5% CO2. At 85-90% confluence, myoblast differentiation was induced by incubation for 96 h in differentiation medium (DMEM supplemented with 4% heat-inactivated horse serum) to form myotubes. Preconditioned medium from cultures of Lewis lung carcinoma cells (obtained from National Institute of Cancer, Frederick, MD) or non-tumorigenic human lung epithelial cell line NL20 (obtained from American Type Culture Collection) that were cultured for 48 h were centrifuged and the supernatant was used to treat C2C12 myotubes (25% final volume in fresh medium) when indicated. Pretreatment of SB202190 or compound C (10 μM, dissolved in DMSO with 0.1% final concentration, Sigma-Aldrich, St. Louis, MO) for 30 min was carried out when indicated. All cell culture experiments were independently replicated 3 times as indicated (N = 3).

Animal use

Experimental protocols were approved in advance by the institutional Animal Welfare Committee at the University of Texas Health Science Center at Houston. For LLC cell xenograft, 100 (l LLC (National Institute of Cancer) cells (1 × 106 cells), or an equal volume of vehicle (PBS) was injected subcutaneously into the right flanks of 7-week-old male C57BL/6 mice (The Jackson Laboratory, Bar Harbor, ME), C/EBPβ-/- mice in C57BL/6 background that were bred from C/EBPβ-/+ mice 56 or mice with muscle-specific knockout of p38β (p38β MKO) 28. The latter were created by crossbreeding floxed-p38β mice (p38β f/f) in C57BL/6 background 30 with muscle creatine kinase-Cre (MCK-Cre, The Jackson Laboratory, Bar Harbor, ME). SB202190 was i.p. injected (5 mg/kg) daily from day 7 of tumor implant. Mice were euthanized on day 21 for evaluation of muscle wasting. When indicated plasmids encoding constitutively active mutant of p38 MAPK isoforms and GFP-LC3 fusion protein 55 were transfected into TA by electroporation as previously described 29.

Transfection of siRNA and plasmids in C2C12 myoblasts

Predesigned siRNAs specific for C/EBPβ, p38α and p38β were purchased form Sigma-Aldrich. The IDs of the siRNAs were SASI_Mm01_00187563, SASI_Mm01_00020743 and SASI_Mm01_00044863, respectively. Control siRNA was purchased from Invitrogen. These siRNAs were introduced into C2C12 myoblasts using the jetPRIME reagent (Polyplus-transfection Inc., Illkirch, France) according to the manufacturer’s protocol. In 24 h, myoblasts were differentiated and experiments were started in another 96 h when myotubes were formed. Plasmids encoding constitutively active p38α and p38β isoforms 57 were transfected into C2C12 myoblasts using the jetPRIME reagent. Empty vector was transfected as the control. These manipulation of p38 MAPK in myoblasts did not alter the end result of differentiation and formation of myotubes 29.

Real-time PCR

Total RNA was isolated from myotubes or muscle by using TRIzol reagent (Invitrogen, Carlsbad, CA). Real-time PCR was performed as described previously 21. Sequences of specific primers are listed in Table 1. Data were normalized to GAPDH. TABLE 1. PCR primers used in this study.

Western blot analysis

Western blot analysis was carried out as described previously 24. Antibodies to total and/or phosphorylated p38MAPK (T181/Y182), p-C/EBPβ (T188), p-ULK1 (S555), total and phosphorylated AMPK (T172), p62 as well as p38α and p38β were from Cell Signaling Technology (Beverly, MA). Antibody to C/EBPβ and ULK1 were from Santa Cruz Biotechnology (Santa Cruz, CA). Antibody to atrogin1/MAFbx was from ECM Biosciences (Versailles, KY). Antibodies to UBR2 and LC3-II were obtained from Novus Biologicals (Littleton, CO). Anti-MHC antibody (MF-20) was from R&D Systems (Minneapolis, MN). Antibody to the HA tag was from Covance (Princeton, NJ, USA). Data was normalized to α-Tubulin (antibody was from Development Studies Hybridoma Bank at the University of Iowa, Iowa City, IA) or GAPDH (Antibody was from Millipore, Billerica, MA, USA). Levels of phosphorylated proteins were normalized to corresponding total proteins.

Chromosome immunoprecipitation (ChIP) assay

ChIP assay was performed as previously described 21. Antibody against C/EBPβ was from Santa Cruz Biotechnology. Pre-immune IgG was from Sigma-Aldrich. The PCR primers used are listed in Table 1.

Histology and confocal microscopy studies

Cross sections of TA were fixed and stained with H&E by the Histology Core at Lester and Sue Smith Breast Center, Baylor College of Medicine. Cross-sectional area of stained muscle sections was quantified by using the ImageJ software (NIH). Five view-fields with ~100 myofibers per field in each section were measured. Frozen sections of mouse TA (5 μm) that expressed GFP-LC3 and/or p38 MAPK mutant were stained with DAPI and examined with a Nikon A1R Confocal Laser Microscope using 60X objective. Adjustment of brightness, contrast, color balance, and final image size was achieved using Adobe Photoshop CS (Adobe Systems, San Jose, CA, USA).

Mapping of phosphorylated amino acid residues in ULK-1

HEK293T cells (American Type Culture Collection, Manassas, VA, USA) cultured in 150 mm plates that were ~50% confluent were co-transfected with a plasmid encoding mouse ULK-1 with a FLAG tag (Addgene) and a plasmid encoding constitutively active p38β 58 (10 μg each) using the jetPRIME reagent (Polyplus-transfection Inc., Illkirch, France). The cell culture medium was replaced with fresh medium at 24 h. After an additional incubation of 24 h cells were lysed in RIPA buffer (50 mM Tris- HCl (pH 7.5), 150 mM NaCl, 2 mM EDTA, 1% NP-40, 0.1% SDS, 2 mM phenylmethylsulphonylfluoride (PMSF), 0.5% sodium deoxycholate, 1 mM NaF, 1/100 protease inhibitor cocktail, and 1/100 phosphatase inhibitor cocktail (Sigma-Aldrich, St. Louis, MO, USA). ULK-1 in cell lysates was precipitated using FLAG-M2 magnetic beads (Sigma-Aldrich) and subjected to 10% SDS-PAGE. The gel was then stained with Coommassie Blue R-250. The ULK1 band was cut out and subjected to tryptic phosphopeptide mapping conducted by Taplin Mass Spectrometry Facility at Harvard Medical School using an LTQ-Orbitrap mass spectrometer (Thermo Electron, West Palm Beach, FL, USA).

Statistical analysis

Data are presented as the mean ± S.D. and were analyzed with one-way ANOVA or Student t test using the SigmaStat software (Systat Software, San Jose, CA) as indicated. When applicable, control samples from independent experiments were normalized to a value of 1 without showing variations (actual variations were within a normal range). Chi-square analysis was carried out by using R to compare the distributions of muscle fiber cross-sectional area among various groups. A p value < 0.05 was considered to be statistically significant. Click here for supplemental data file.

SUPPLEMENTAL MATERIAL

All supplemental data for this article are also available online at http://www.cell-stress.com/researcharticles/p38%ce%b2-mapk-mediates-ulk1-dependent-induction-of-autophagy-in-skeletal-muscle-of-tumor-bearing-mice/.

Table 1

TABLE 1. PCR primers used in this study.

Primer	Sequence
C/EBPβ forward	5′-GACAAGCTGAGCGACGAGTACA
C/EBPβ reverse	5′-CGACAGCTGCTCCACCTTCTTC
LC3b forward	5’-CGTCCTGGACAAGACCAAGT
LC3b reverse	5’-ATTGCTGTCCCGAATGTCTC
GABARAPL1 forward	5’-CATCGTGGAGAAGGCTCCTA
GABARAPL1 reverse	5’-ATACAGCTGGCCCATGGTAG
Atg12l forward	5’-GGCCTCGGAACAGTTGTTTA
Atg12l reverse	5’-CAGCACCGAAATGTCTCTGA
Beclin1 forward	5’-GGCCAATAAGATGGGTCTGA
Beclin1 reverse	5’-CACTGCCTCCAGTGTCTTCA
Atg4b forward	5’-ATTGCTGTGGGGTTTTTCTG
Atg4b reverse	5’-AACCCCAGGATTTTCAGAGG
GAPDH forward	5’-CATGGCCTTCCGTGTTCCTA
GAPDH reverse	5’-GCGGCACGTCAGATCCA	Product size
LC3b -122 forward	5’-GACAGTTAACAGATGCTC	198 bp
LC3b -122 reverse	5’-AGTCCGCAGCCGAGTCAG
LC3b -347 forward	5’-GAGCCACAAGATCAGATC	195 bp
LC3b -347 reverse	5’-TCATTCCCCTTCAGTCCT
LC3b -711 forward	5’-TGATTGCTCACCAACCAA	198 bp
LC3b -711 reverse	5’-GACAACACCTGCTGTGCA
Gabarapl1 -191 forward	5’-AACTACCCTACAGGTGAT	201 bp
Gabarapl1 -191 reverse	5’-CATCAAGGTTAGAAGAAG
Gabarapl1 -398 forward	5’-CTTATAAAATGAATGGAT	199 bp
Gabarapl1 -398 reverse	5’-CTCCTTCTGACTGGTGTC
Gabarapl1 -618 forward	5’-CATAAGGACACCAGTCAG	205 bp
Gabarapl1 -618 reverse	5’-GATGCCCAAAACAAACAC
Gabarapl1 -829 forward	5’-CATTGCTCTGGAAACAGC	197 bp
Gabarapl1 -829 reverse	5’-CCAAGCTTTTCCTAAACC

15 in total

1. Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)¹.

Authors: Daniel J Klionsky; Amal Kamal Abdel-Aziz; Sara Abdelfatah; Mahmoud Abdellatif; Asghar Abdoli; Steffen Abel; Hagai Abeliovich; Marie H Abildgaard; Yakubu Princely Abudu; Abraham Acevedo-Arozena; Iannis E Adamopoulos; Khosrow Adeli; Timon E Adolph; Annagrazia Adornetto; Elma Aflaki; Galila Agam; Anupam Agarwal; Bharat B Aggarwal; Maria Agnello; Patrizia Agostinis; Javed N Agrewala; Alexander Agrotis; Patricia V Aguilar; S Tariq Ahmad; Zubair M Ahmed; Ulises Ahumada-Castro; Sonja Aits; Shu Aizawa; Yunus Akkoc; Tonia Akoumianaki; Hafize Aysin Akpinar; Ahmed M Al-Abd; Lina Al-Akra; Abeer Al-Gharaibeh; Moulay A Alaoui-Jamali; Simon Alberti; Elísabet Alcocer-Gómez; Cristiano Alessandri; Muhammad Ali; M Abdul Alim Al-Bari; Saeb Aliwaini; Javad Alizadeh; Eugènia Almacellas; Alexandru Almasan; Alicia Alonso; Guillermo D Alonso; Nihal Altan-Bonnet; Dario C Altieri; Élida M C Álvarez; Sara Alves; Cristine Alves da Costa; Mazen M Alzaharna; Marialaura Amadio; Consuelo Amantini; Cristina Amaral; Susanna Ambrosio; Amal O Amer; Veena Ammanathan; Zhenyi An; Stig U Andersen; Shaida A Andrabi; Magaiver Andrade-Silva; Allen M Andres; Sabrina Angelini; David Ann; Uche C Anozie; Mohammad Y Ansari; Pedro Antas; Adam Antebi; Zuriñe Antón; Tahira Anwar; Lionel Apetoh; Nadezda Apostolova; Toshiyuki Araki; Yasuhiro Araki; Kohei Arasaki; Wagner L Araújo; Jun Araya; Catherine Arden; Maria-Angeles Arévalo; Sandro Arguelles; Esperanza Arias; Jyothi Arikkath; Hirokazu Arimoto; Aileen R Ariosa; Darius Armstrong-James; Laetitia Arnauné-Pelloquin; Angeles Aroca; Daniela S Arroyo; Ivica Arsov; Rubén Artero; Dalia Maria Lucia Asaro; Michael Aschner; Milad Ashrafizadeh; Osnat Ashur-Fabian; Atanas G Atanasov; Alicia K Au; Patrick Auberger; Holger W Auner; Laure Aurelian; Riccardo Autelli; Laura Avagliano; Yenniffer Ávalos; Sanja Aveic; Célia Alexandra Aveleira; Tamar Avin-Wittenberg; Yucel Aydin; Scott Ayton; Srinivas Ayyadevara; Maria Azzopardi; Misuzu Baba; Jonathan M Backer; Steven K Backues; Dong-Hun Bae; 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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; 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Bruno J de Andrade Silva; Johnatas D Silva; Eduardo Silva-Pavez; Sandrine Silvente-Poirot; Rachel E Simmonds; Anna Katharina Simon; Hans-Uwe Simon; Matias Simons; Anurag Singh; Lalit P Singh; Rajat Singh; Shivendra V Singh; Shrawan K Singh; Sudha B Singh; Sunaina Singh; Surinder Pal Singh; Debasish Sinha; Rohit Anthony Sinha; Sangita Sinha; Agnieszka Sirko; Kapil Sirohi; Efthimios L Sivridis; Panagiotis Skendros; Aleksandra Skirycz; Iva Slaninová; Soraya S Smaili; Andrei Smertenko; Matthew D Smith; Stefaan J Soenen; Eun Jung Sohn; Sophia P M Sok; Giancarlo Solaini; Thierry Soldati; Scott A Soleimanpour; Rosa M Soler; Alexei Solovchenko; Jason A Somarelli; Avinash Sonawane; Fuyong Song; Hyun Kyu Song; Ju-Xian Song; Kunhua Song; Zhiyin Song; Leandro R Soria; Maurizio Sorice; Alexander A Soukas; Sandra-Fausia Soukup; Diana Sousa; Nadia Sousa; Paul A Spagnuolo; Stephen A Spector; M M Srinivas Bharath; Daret St Clair; Venturina Stagni; Leopoldo Staiano; Clint A Stalnecker; Metodi V Stankov; Peter B Stathopulos; Katja Stefan; Sven Marcel Stefan; Leonidas Stefanis; Joan S Steffan; Alexander Steinkasserer; Harald Stenmark; Jared Sterneckert; Craig Stevens; Veronika Stoka; Stephan Storch; Björn Stork; Flavie Strappazzon; Anne Marie Strohecker; Dwayne G Stupack; Huanxing Su; Ling-Yan Su; Longxiang Su; Ana M Suarez-Fontes; Carlos S Subauste; Selvakumar Subbian; Paula V Subirada; Ganapasam Sudhandiran; Carolyn M Sue; Xinbing Sui; Corey Summers; Guangchao Sun; Jun Sun; Kang Sun; Meng-Xiang Sun; Qiming Sun; Yi Sun; Zhongjie Sun; Karen K S Sunahara; Eva Sundberg; Katalin Susztak; Peter Sutovsky; Hidekazu Suzuki; Gary Sweeney; J David Symons; Stephen Cho Wing Sze; Nathaniel J Szewczyk; Anna Tabęcka-Łonczynska; Claudio Tabolacci; Frank Tacke; Heinrich Taegtmeyer; Marco Tafani; Mitsuo Tagaya; Haoran Tai; Stephen W G Tait; Yoshinori Takahashi; Szabolcs Takats; Priti Talwar; Chit Tam; Shing Yau Tam; Davide Tampellini; Atsushi Tamura; Chong Teik Tan; Eng-King Tan; Ya-Qin Tan; Masaki Tanaka; Motomasa Tanaka; Daolin Tang; Jingfeng Tang; Tie-Shan Tang; Isei Tanida; Zhipeng Tao; Mohammed Taouis; Lars Tatenhorst; Nektarios Tavernarakis; Allen Taylor; Gregory A Taylor; Joan M Taylor; Elena Tchetina; Andrew R Tee; Irmgard Tegeder; David Teis; Natercia Teixeira; Fatima Teixeira-Clerc; Kumsal A Tekirdag; Tewin Tencomnao; Sandra Tenreiro; Alexei V Tepikin; Pilar S Testillano; Gianluca Tettamanti; Pierre-Louis Tharaux; Kathrin Thedieck; Arvind A Thekkinghat; Stefano Thellung; Josephine W Thinwa; V P Thirumalaikumar; Sufi Mary Thomas; Paul G Thomes; Andrew Thorburn; Lipi Thukral; Thomas Thum; Michael Thumm; Ling Tian; Ales Tichy; Andreas Till; Vincent Timmerman; Vladimir I Titorenko; Sokol V Todi; Krassimira Todorova; Janne M Toivonen; Luana Tomaipitinca; Dhanendra Tomar; Cristina Tomas-Zapico; Sergej Tomić; Benjamin Chun-Kit Tong; Chao Tong; Xin Tong; Sharon A Tooze; Maria L Torgersen; Satoru Torii; Liliana Torres-López; Alicia Torriglia; Christina G Towers; Roberto Towns; Shinya Toyokuni; Vladimir Trajkovic; Donatella Tramontano; Quynh-Giao Tran; Leonardo H Travassos; Charles B Trelford; Shirley Tremel; Ioannis P Trougakos; Betty P Tsao; Mario P Tschan; Hung-Fat Tse; Tak Fu Tse; Hitoshi Tsugawa; Andrey S Tsvetkov; David A Tumbarello; Yasin Tumtas; María J Tuñón; Sandra Turcotte; Boris Turk; Vito Turk; Bradley J Turner; Richard I Tuxworth; Jessica K Tyler; Elena V Tyutereva; Yasuo Uchiyama; Aslihan Ugun-Klusek; Holm H Uhlig; Marzena Ułamek-Kozioł; Ilya V Ulasov; Midori Umekawa; Christian Ungermann; Rei Unno; Sylvie Urbe; Elisabet Uribe-Carretero; Suayib Üstün; Vladimir N Uversky; Thomas Vaccari; Maria I Vaccaro; Björn F Vahsen; Helin Vakifahmetoglu-Norberg; Rut Valdor; Maria J Valente; Ayelén Valko; Richard B Vallee; Angela M Valverde; Greet Van den Berghe; Stijn van der Veen; Luc Van Kaer; Jorg van Loosdregt; Sjoerd J L van Wijk; Wim Vandenberghe; Ilse Vanhorebeek; Marcos A Vannier-Santos; Nicola Vannini; M Cristina Vanrell; Chiara Vantaggiato; Gabriele Varano; Isabel Varela-Nieto; 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; Alexander J Whitworth; Katarzyna Wiktorska; Manon E Wildenberg; Tom Wileman; Simon Wilkinson; Dieter Willbold; Brett Williams; Robin S B Williams; Roger L Williams; Peter R Williamson; Richard A Wilson; Beate Winner; Nathaniel J Winsor; Steven S Witkin; Harald Wodrich; Ute Woehlbier; Thomas Wollert; Esther Wong; Jack Ho Wong; Richard W Wong; Vincent Kam Wai Wong; W Wei-Lynn Wong; An-Guo Wu; Chengbiao Wu; Jian Wu; Junfang Wu; Kenneth K Wu; Min Wu; Shan-Ying Wu; Shengzhou Wu; Shu-Yan Wu; Shufang Wu; William K K Wu; Xiaohong Wu; Xiaoqing Wu; Yao-Wen Wu; Yihua Wu; Ramnik J Xavier; Hongguang Xia; Lixin Xia; Zhengyuan Xia; Ge Xiang; Jin Xiang; Mingliang Xiang; Wei Xiang; Bin Xiao; Guozhi Xiao; Hengyi Xiao; Hong-Tao Xiao; Jian Xiao; Lan Xiao; Shi Xiao; Yin Xiao; Baoming Xie; Chuan-Ming Xie; Min Xie; Yuxiang Xie; Zhiping Xie; Zhonglin Xie; Maria Xilouri; Congfeng Xu; En Xu; Haoxing Xu; Jing Xu; JinRong Xu; Liang Xu; Wen Wen Xu; Xiulong Xu; Yu Xue; Sokhna M S Yakhine-Diop; Masamitsu Yamaguchi; Osamu Yamaguchi; Ai Yamamoto; Shunhei Yamashina; Shengmin Yan; Shian-Jang Yan; Zhen Yan; Yasuo Yanagi; Chuanbin Yang; Dun-Sheng Yang; Huan Yang; Huang-Tian Yang; Hui Yang; Jin-Ming Yang; Jing Yang; Jingyu Yang; Ling Yang; Liu Yang; Ming Yang; Pei-Ming Yang; Qian Yang; Seungwon Yang; Shu Yang; Shun-Fa Yang; Wannian Yang; Wei Yuan Yang; Xiaoyong Yang; Xuesong Yang; Yi Yang; Ying Yang; Honghong Yao; Shenggen Yao; Xiaoqiang Yao; Yong-Gang Yao; Yong-Ming Yao; Takahiro Yasui; Meysam Yazdankhah; Paul M Yen; Cong Yi; Xiao-Ming Yin; Yanhai Yin; Zhangyuan Yin; Ziyi Yin; Meidan Ying; Zheng Ying; Calvin K Yip; Stephanie Pei Tung Yiu; Young H Yoo; Kiyotsugu Yoshida; Saori R Yoshii; Tamotsu Yoshimori; Bahman Yousefi; Boxuan Yu; Haiyang Yu; Jun Yu; Jun Yu; Li Yu; Ming-Lung Yu; Seong-Woon Yu; Victor C Yu; W Haung Yu; Zhengping Yu; Zhou Yu; Junying Yuan; Ling-Qing Yuan; Shilin Yuan; Shyng-Shiou F Yuan; Yanggang Yuan; Zengqiang Yuan; Jianbo Yue; Zhenyu Yue; Jeanho Yun; Raymond L Yung; David N Zacks; Gabriele Zaffagnini; Vanessa O Zambelli; Isabella Zanella; Qun S Zang; Sara Zanivan; Silvia Zappavigna; Pilar Zaragoza; Konstantinos S Zarbalis; Amir Zarebkohan; Amira Zarrouk; Scott O Zeitlin; Jialiu Zeng; Ju-Deng Zeng; Eva Žerovnik; Lixuan Zhan; Bin Zhang; Donna D Zhang; Hanlin Zhang; Hong Zhang; Hong Zhang; Honghe Zhang; Huafeng Zhang; Huaye Zhang; Hui Zhang; Hui-Ling Zhang; Jianbin Zhang; Jianhua Zhang; Jing-Pu Zhang; Kalin Y B Zhang; Leshuai W Zhang; Lin Zhang; Lisheng Zhang; Lu Zhang; Luoying Zhang; Menghuan Zhang; Peng Zhang; Sheng Zhang; Wei Zhang; Xiangnan Zhang; Xiao-Wei Zhang; Xiaolei Zhang; Xiaoyan Zhang; Xin Zhang; Xinxin Zhang; Xu Dong Zhang; Yang Zhang; Yanjin Zhang; Yi Zhang; Ying-Dong Zhang; Yingmei Zhang; Yuan-Yuan Zhang; Yuchen Zhang; Zhe Zhang; Zhengguang Zhang; Zhibing Zhang; Zhihai Zhang; Zhiyong Zhang; Zili Zhang; Haobin Zhao; Lei Zhao; Shuang Zhao; Tongbiao Zhao; Xiao-Fan Zhao; Ying Zhao; Yongchao Zhao; Yongliang Zhao; Yuting Zhao; Guoping Zheng; Kai Zheng; Ling Zheng; Shizhong Zheng; 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

Review 2. Cancer Takes a Toll on Skeletal Muscle by Releasing Heat Shock Proteins-An Emerging Mechanism of Cancer-Induced Cachexia.

Authors: Thomas K Sin; Guohua Zhang; Zicheng Zhang; Song Gao; Min Li; Yi-Ping Li
Journal: Cancers (Basel) Date: 2019-08-30 Impact factor: 6.639

3. HCT116 colorectal liver metastases exacerbate muscle wasting in a mouse model for the study of colorectal cancer cachexia.

Authors: Joshua R Huot; Leah J Novinger; Fabrizio Pin; Andrea Bonetto
Journal: Dis Model Mech Date: 2020-01-24 Impact factor: 5.758

4. Androgen depletion alters the diurnal patterns to signals that regulate autophagy in the limb skeletal muscle.

Authors: Michael L Rossetti; Robert J Tomko; Bradley S Gordon
Journal: Mol Cell Biochem Date: 2020-10-31 Impact factor: 3.396

Review 5. Management of Cancer Cachexia: Attempting to Develop New Pharmacological Agents for New Effective Therapeutic Options.

Authors: Gioacchino P Marceca; Priya Londhe; Federica Calore
Journal: Front Oncol Date: 2020-03-04 Impact factor: 6.244

p38β MAPK mediates ULK1-dependent induction of autophagy in skeletal muscle of tumor-bearing mice.

INTRODUCTION

RESULTS

LLC induces autophagy activation in skeletal muscle cells through p38β MAPK

FIGURE 1: p38β MAPK activation is necessary and sufficient for autophagy activation by tumor in skeletal muscle cells.

LLC induces muscle wasting through p38β MAPK-mediated activation of autophagy and UPP

FIGURE 2: Muscle-specific knockout of p38β MAPK abrogates activation of autophagy, UPP and muscle wasting in tumor-bearing mice.

p38β MAPK-mediated C/EBPβ activation is critical to LLC-induced autophagy activation

FIGURE 3: The p38β MAPK → C/EBPβ signaling pathway mediates autophagy activation by tumor in skeletal muscle cells.

p38β MAPK → C/EBPβ signaling mediates upregulation of specific autophagy-related genes

FIGURE 4. C/EBPβ mediates tumor induction of autophagy-related genes in skeletal muscle cells.

FIGURE 5: p38β MAPK is required for upregulation of C/EBPβ-responsive autophagy-related genes in cachectic muscle of tumor-bearing mice.

LLC induces ULK1 activation in skeletal muscle through p38β MAPK

FIGURE 6: p38β MAPK activates ULK1 in skeletal muscle cells in response to tumor.

DISCUSSION

MATERIALS AND METHODS

Myogenic cell culture

Animal use

Transfection of siRNA and plasmids in C2C12 myoblasts

Real-time PCR

Western blot analysis

Chromosome immunoprecipitation (ChIP) assay

Histology and confocal microscopy studies

Mapping of phosphorylated amino acid residues in ULK-1

Statistical analysis

SUPPLEMENTAL MATERIAL

1. Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)¹.

Review 2. Cancer Takes a Toll on Skeletal Muscle by Releasing Heat Shock Proteins-An Emerging Mechanism of Cancer-Induced Cachexia.

3. HCT116 colorectal liver metastases exacerbate muscle wasting in a mouse model for the study of colorectal cancer cachexia.

4. Androgen depletion alters the diurnal patterns to signals that regulate autophagy in the limb skeletal muscle.

Review 5. Management of Cancer Cachexia: Attempting to Develop New Pharmacological Agents for New Effective Therapeutic Options.

Review 6. p38β and Cancer: The Beginning of the Road.

7. Programmed Cell Death in the Left and Right Ventricle of the Late Phase of Post-Infarction Heart Failure.

8. Weight Loss in Cancer Patients Correlates With p38β MAPK Activation in Skeletal Muscle.

9. Wheel running improves fasting-induced AMPK signaling in skeletal muscle from tumor-bearing mice.

Review 10. Immunometabolism: new insights and lessons from antigen-directed cellular immune responses.

p38β MAPK mediates ULK1-dependent induction of autophagy in skeletal muscle of tumor-bearing mice.

INTRODUCTION

RESULTS

LLC induces autophagy activation in skeletal muscle cells through p38β MAPK

FIGURE 1: p38β MAPK activation is necessary and sufficient for autophagy activation by tumor in skeletal muscle cells.

LLC induces muscle wasting through p38β MAPK-mediated activation of autophagy and UPP

FIGURE 2: Muscle-specific knockout of p38β MAPK abrogates activation of autophagy, UPP and muscle wasting in tumor-bearing mice.

p38β MAPK-mediated C/EBPβ activation is critical to LLC-induced autophagy activation

FIGURE 3: The p38β MAPK → C/EBPβ signaling pathway mediates autophagy activation by tumor in skeletal muscle cells.

p38β MAPK → C/EBPβ signaling mediates upregulation of specific autophagy-related genes

FIGURE 4. C/EBPβ mediates tumor induction of autophagy-related genes in skeletal muscle cells.

FIGURE 5: p38β MAPK is required for upregulation of C/EBPβ-responsive autophagy-related genes in cachectic muscle of tumor-bearing mice.

LLC induces ULK1 activation in skeletal muscle through p38β MAPK

FIGURE 6: p38β MAPK activates ULK1 in skeletal muscle cells in response to tumor.

DISCUSSION

MATERIALS AND METHODS

Myogenic cell culture

Animal use

Transfection of siRNA and plasmids in C2C12 myoblasts

Real-time PCR

Western blot analysis

Chromosome immunoprecipitation (ChIP) assay

Histology and confocal microscopy studies

Mapping of phosphorylated amino acid residues in ULK-1

Statistical analysis

SUPPLEMENTAL MATERIAL

1. Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)1.

Review 2. Cancer Takes a Toll on Skeletal Muscle by Releasing Heat Shock Proteins-An Emerging Mechanism of Cancer-Induced Cachexia.

3. HCT116 colorectal liver metastases exacerbate muscle wasting in a mouse model for the study of colorectal cancer cachexia.

4. Androgen depletion alters the diurnal patterns to signals that regulate autophagy in the limb skeletal muscle.

Review 5. Management of Cancer Cachexia: Attempting to Develop New Pharmacological Agents for New Effective Therapeutic Options.

Review 6. p38β and Cancer: The Beginning of the Road.

7. Programmed Cell Death in the Left and Right Ventricle of the Late Phase of Post-Infarction Heart Failure.

8. Weight Loss in Cancer Patients Correlates With p38β MAPK Activation in Skeletal Muscle.

9. Wheel running improves fasting-induced AMPK signaling in skeletal muscle from tumor-bearing mice.

Review 10. Immunometabolism: new insights and lessons from antigen-directed cellular immune responses.

1. Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)¹.