Hepatitis B virus–triggered autophagy targets TNFRSF10B/death receptor 5 for degradation to limit TNFSF10/TRAIL response

Shin, Gu Choul; Kang, Hong Seok; Lee, Ah Ram; Kim, Kyun-Hwan

doi:10.1080/15548627.2016.1239002

Cited by 53 publications

(51 citation statements)

References 60 publications

(87 reference statements)

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“…In line with this hypothesis, knockdown of LC3B led to a~40% reduction of Tginduced cell death and a~30% reduction of Tg-induced PARP cleavage in LNCaP cells ( Fig Combined silencing of LC3A and LC3B did not produce any further reduction in Tg-induced cell death compared to that observed upon silencing of LC3B alone (data not shown). Hepatitis B virus-induced autophagy can trigger LC3B-dependent degradation of DR5 [66]. However, and in accordance with Tg blocking functional autophagy [33], knockdown of LC3B did not result in higher DR5 protein levels in Tg-treated cells (Additional file 2: Figure S7, C-F).…”

Section: A Non-autophagic Function Of Lc3b Is Partially Required Formentioning

confidence: 53%

Cell death induced by the ER stressor thapsigargin involves death receptor 5, a non-autophagic function of MAP1LC3B, and distinct contributions from unfolded protein response components

et al. 2020

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Background: Cell death triggered by unmitigated endoplasmic reticulum (ER) stress plays an important role in physiology and disease, but the death-inducing signaling mechanisms are incompletely understood. To gain more insight into these mechanisms, the ER stressor thapsigargin (Tg) is an instrumental experimental tool. Additionally, Tg forms the basis for analog prodrugs designed for cell killing in targeted cancer therapy. Tg induces apoptosis via the unfolded protein response (UPR), but how apoptosis is initiated, and how individual effects of the various UPR components are integrated, is unclear. Furthermore, the role of autophagy and autophagy-related (ATG) proteins remains elusive.Methods: To systematically address these key questions, we analyzed the effects of Tg and therapeutically relevant Tg analogs in two human cancer cell lines of different origin (LNCaP prostate-and HCT116 colon cancer cells), using RNAi and inhibitory drugs to target death receptors, UPR components and ATG proteins, in combination with measurements of cell death by fluorescence imaging and propidium iodide staining, as well as real-time RT-PCR and western blotting to monitor caspase activity, expression of ATG proteins, UPR components, and downstream ER stress signaling.Results: In both cell lines, Tg-induced cell death depended on death receptor 5 and caspase-8. Optimal cytotoxicity involved a non-autophagic function of MAP1LC3B upstream of procaspase-8 cleavage. PERK, ATF4 and CHOP were required for Tg-induced cell death, but surprisingly acted in parallel rather than as a linear pathway; ATF4 and CHOP were independently required for Tg-mediated upregulation of death receptor 5 and MAP1LC3B proteins, whereas PERK acted via other pathways. Interestingly, IRE1 contributed to Tg-induced cell death in a cell typespecific manner. This was linked to an XBP1-dependent activation of c-Jun N-terminal kinase, which was proapoptotic in LNCaP but not HCT116 cells. Molecular requirements for cell death induction by therapy-relevant Tg analogs were identical to those observed with Tg. Conclusions: Together, our results provide a new, integrated understanding of UPR signaling mechanisms and downstream mediators that induce cell death upon Tg-triggered, unmitigated ER stress.

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Section: A Non-autophagic Function Of Lc3b Is Partially Required Formentioning

confidence: 53%

Cell death induced by the ER stressor thapsigargin involves death receptor 5, a non-autophagic function of MAP1LC3B, and distinct contributions from unfolded protein response components

et al. 2020

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“…17 HBx also promotes autophagic and lysosomal degradation of the TNFSF10/TRAIL (tumor necrosis factor related apoptosis-inducing ligand) death receptors, supporting survival of HBV-infected cells and evading antiviral immunity. 18 In fact, HBx stimulates Parkin-mediated mitophagy and suppresses mitochondrial apoptosis, a mechanism which may contribute to HBV-induced hepatocarcionogenesis. 19…”

Section: Apoptosismentioning

confidence: 99%

Cell Death and Liver Disease

2020

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Cell death is now reclassified into several types based on the mechanisms and morphologic phenotype. Understanding of such classifications offers insights into the pathogenesis of liver disease, as well as diagnostic or therapeutic implications. Apoptosis is recognized relatively easily due to its unique morphology, but lytic cell death may occur in the form of accidental necrosis, mitochondria permeability transitiondriven necrosis, necroptosis, pyroptosis, ferroptosis, and parthanatos. The cell may be engulfed by neighboring cells due to a loss of integrin signaling or cancer cell competition by entosis, a type of cell death. The classification also includes mechanistically termed cell death such as autophagy-dependent cell death and lysosome-dependent cell death. These different types of cell death may occur uniquely in certain liver diseases but may coexist in the evolution of the disease. They occur in parenchymal and non-parenchymal liver cells, as well as inflammatory cells, causing distinct pathologic consequences. This review briefly covers the recently revised classifications of cell death and discusses their relevance to liver diseases of different etiologies.

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“…CCND2 regulated HBV replication via enhancing the acivity of HBV core promoters . TNFSF10 has been reported to paticipate in HBV evasion through HBX‐induced autophagy . SUZ12 was activated during both HBV replication and liver carcinogenesis .…”

Section: Discussionmentioning

confidence: 99%

Alteration of microRNA profiles by a novel inhibitor of human La protein in HBV‐transformed human hepatoma cells

Pan

Tong

Tang

2017

Journal of Medical Virology

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A pyrazolopyridine HBSC11 was previously identified as a novel inhibitor of human La protein with anti‐hepatitis B virus (HBV) activity. However, the underlying mechanism(s) of HBV inhibition by HBSC11 remains unclear. This study aimed to examine the regulation of microRNA (miRNA) by HBSC11 in HBV‐transformed human hepatoma HepG2.2.15 cells using microarray and quantitative real‐time PCR. Target genes of the differentially expressed miRNAs were predicted and subjected to bioinformatics analysis. Results showed that HBSC11 significantly upregulated the expression of miR‐3912‐5p, miR‐6793‐5p, and miR‐7159‐5p in HepG2.2.15 cells. Target genes of the three miRNAs were mainly involved in the regulation of nucleic acid‐templated transcription, negative regulation of gene expression, nucleic acid binding transcription factor activity and regulation of phosphorylation. In addition, target genes were enriched in certain regulatory pathways related to HBV infection and HBV‐associated disease progression, such as the transforming growth factor (TGF)‐β, Wnt, and p53 signaling. Our study demonstrates the involvement of miR‐3912‐5p, miR‐6793‐5p, and miR‐7159‐5p and the potential modulation of specific pathways (TGF‐β, Wnt, and p53 signaling) in HBSC11‐mediated inhibition of HBV replication. This study provides insight into the molecular mechanism of the action of HBSC11 against HBV infection and will support the development of antiviral drugs targeting La protein.

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Hepatitis B virus–triggered autophagy targets TNFRSF10B/death receptor 5 for degradation to limit TNFSF10/TRAIL response

Cited by 53 publications

References 60 publications

Cell death induced by the ER stressor thapsigargin involves death receptor 5, a non-autophagic function of MAP1LC3B, and distinct contributions from unfolded protein response components

Cell death induced by the ER stressor thapsigargin involves death receptor 5, a non-autophagic function of MAP1LC3B, and distinct contributions from unfolded protein response components

Cell Death and Liver Disease

Alteration of microRNA profiles by a novel inhibitor of human La protein in HBV‐transformed human hepatoma cells

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