Your search keyword '"Chan Hoon Jung"' showing total 5 results

1. The N-degron pathway mediates the autophagic degradation of cytosolic mitochondrial DNA during sterile innate immune responses

Author

Chan Hoon Jung, Yoon Jee Lee, Eun Hye Cho, Gee Eun Lee, Sung Tae Kim, Ki Sa Sung, Daeho Kim, Dong Hyun Kim, Yeon Sung Son, Jin-Hyun Ahn, Dohyun Han, and Yong Tae Kwon

Subjects

CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: The human body reacts to tissue damage by generating damage-associated molecular patterns (DAMPs) that activate sterile immune responses. To date, little is known about how DAMPs are removed to avoid excessive immune responses. Here, we show that proteasomal dysfunction induces the release of mitochondrial DNA (mtDNA) as a DAMP that activates the cyclic GMP-AMP synthase (cGAS)-stimulator of interferon gene (STING) pathway and is subsequently degraded through the N-degron pathway. In the resolution phase of sterile immune responses, DNA-dependent protein kinase (DNA-PK) senses cytosolic mtDNA and activates N-terminal (Nt-) arginylation by ATE1 R-transferases. The substrates of Nt-arginylation include the molecular chaperone BiP/GRP78 retrotranslocated from the endoplasmic reticulum (ER). R-BiP, the Nt-arginylated species of BiP, is associated with cytosolic mtDNA to accelerate its targeting to autophagic membranes for lysosomal degradation. Thus, cytosolic mtDNA activates the N-degron pathway to facilitate its own degradation and form a negative feedback loop, by which the cell can turn off sterile immune responses at the right time.

Published

2025

2. Enhancing Bifunctional Electrocatalytic Activities of Oxygen Electrodes via Incorporating Highly Conductive Sm3+ and Nd3+ Double-Doped Ceria for Reversible Solid Oxide Cells

Author

Jeong Hwa Park, Jong-Eun Hong, Kyeong Joon Kim, Chan Hoon Jung, Doyeub Kim, Kang Taek Lee, and Hong Rim Shin

Subjects

Materials science, Hydrogen, Electrolytic cell, Oxygen evolution, Oxide, chemistry.chemical_element, Oxygen, law.invention, chemistry.chemical_compound, chemistry, Chemical engineering, law, Electrode, General Materials Science, Triple phase boundary, Clark electrode

Abstract

Solid oxide cells (SOCs) are mutually convertible energy devices capable of generating electricity from chemical fuels including hydrogen in the fuel cell mode and producing green hydrogen using electricity from renewable but intermittent solar and wind resources in the electrolysis cell mode. An effective approach to enhance the performance of SOCs at reduced temperatures is by developing highly active oxygen electrodes for both oxygen reduction and oxygen evolution reactions. Herein, highly conductive Sm3+ and Nd3+ double-doped ceria (Sm0.075Nd0.075Ce0.85O2-δ, SNDC) is utilized as an active component for reversible SOC applications. We develop a novel La0.6Sr0.4Co0.2Fe0.8O3 -δ (LSCF)-SNDC composite oxygen electrode. Compared with the conventional LSCF-Gd-doped ceria oxygen electrode, the LSCF-SNDC exhibits ∼35% lower cathode polarization resistance (0.042 Ω cm2 at 750 °C) owing to rapid oxygen incorporation and surface diffusion kinetics. Furthermore, the SOC with the LSCF-SNDC oxygen electrode and the SNDC buffer layer yields a remarkable performance in both the fuel cell (1.54 W cm-2 at 750 °C) and electrolysis cell (1.37 A cm-2 at 750 °C) modes because the incorporation of SNDC promotes the surface diffusion kinetics at the oxygen electrode bulk and the activity of the triple phase boundary at the interface. These findings suggest that the highly conductive SNDC material effectively enhances both oxygen reduction and oxygen evolution reactions, thus serving as a promising material in reversible SOC applications at reduced temperatures.

Published

2021

3. Aggresomal sequestration and STUB1-mediated ubiquitylation during mammalian proteaphagy of inhibited proteasomes

Author

Won Choi, Nak Kyoon Kim, Sang Min Lim, Jun Hyoung Jeon, Seoyoung Park, Jung Hoon Lee, Min Jae Lee, Yejin Yun, Dohyun Han, Chan Hoon Jung, Jee Young Lee, Yong Tae Kwon, and Su A. Yang

Subjects

Autophagosome, Proteasome Endopeptidase Complex, Ubiquitin-Protein Ligases, Biochemistry, Proteaphagy, Ubiquitin, aggresome, ubiquitin, Macroautophagy, Sequestosome-1 Protein, Humans, Organelles, STUB1, Multidisciplinary, biology, Chemistry, Autophagy, Ubiquitination, Biological Sciences, HDAC6, proteaphagy, Cell biology, proteasome, Aggresome, Proteasome, A549 Cells, biology.protein

Abstract

Significance The ubiquitin–proteasome system and autophagy are two major intracellular proteolytic pathways, and both remove misfolded and proteotoxic proteins from eukaryotic cells. This study describes the detailed regulatory pathway of proteasome degradation by autophagy for its own quality control. We discovered that a portion of inhibited proteasomes is actively sequestered into the aggresome, an insoluble fraction of the mammalian cell. The aggresome functions as a triage point for proteasome recovery and autophagic degradation. This mainly distinguishes proteasome quality control in mammals from that in other organisms. STUB1/CHIP E3 Ub ligase has a critical role in targeting inhibited proteasomes into the aggresome. These results provide strong insights into protein catabolism in various pathological conditions originating from impaired proteasomes., The 26S proteasome, a self-compartmentalized protease complex, plays a crucial role in protein quality control. Multiple levels of regulatory systems modulate proteasomal activity for substrate hydrolysis. However, the destruction mechanism of mammalian proteasomes is poorly understood. We found that inhibited proteasomes are sequestered into the insoluble aggresome via HDAC6- and dynein-mediated transport. These proteasomes colocalized with the autophagic receptor SQSTM1 and cleared through selective macroautophagy, linking aggresomal segregation to autophagic degradation. This proteaphagic pathway was counterbalanced with the recovery of proteasomal activity and was critical for reducing cellular proteasomal stress. Changes in associated proteins and polyubiquitylation on inhibited 26S proteasomes participated in the targeting mechanism to the aggresome and autophagosome. The STUB1 E3 Ub ligase specifically ubiquitylated purified human proteasomes in vitro, mainly via Lys63-linked chains. Genetic and chemical inhibition of STUB1 activity significantly impaired proteasome processing and reduced resistance to proteasomal stress. These data demonstrate that aggresomal sequestration is the crucial upstream event for proteasome quality control and overall protein homeostasis in mammals.

Published

2020

4. Chemical modulation of SQSTM1/p62-mediated xenophagy that targets a broad range of pathogenic bacteria

Author

Yoon Jee Lee, Jin Kyung Kim, Chan Hoon Jung, Young Jae Kim, Eui Jung Jung, Su Hyun Lee, Ha Rim Choi, Yeon Sung Son, Sang Mi Shim, Sang Min Jeon, Jin Ho Choe, Sang-Hee Lee, Jake Whang, Kyung-Cheol Sohn, Gang Min Hur, Hyun Tae Kim, Jinki Yeom, Eun-Kyeong Jo, and Yong Tae Kwon

Subjects

Salmonella typhimurium, Sirolimus, Ubiquitin, Cell Biology, Mice, Sequestosome-1 Protein, Macroautophagy, Autophagy, BCG Vaccine, Animals, Cytokines, Apoptosis Regulatory Proteins, Molecular Biology, Research Paper

Abstract

The N-degron pathway is a proteolytic system in which the N-terminal degrons (N-degrons) of proteins, such as arginine (Nt-Arg), induce the degradation of proteins and subcellular organelles via the ubiquitin-proteasome system (UPS) or macroautophagy/autophagy-lysosome system (hereafter autophagy). Here, we developed the chemical mimics of the N-degron Nt-Arg as a pharmaceutical means to induce targeted degradation of intracellular bacteria via autophagy, such as Salmonella enterica serovar Typhimurium (S. Typhimurium), Escherichia coli, and Streptococcus pyogenes as well as Mycobacterium tuberculosis (Mtb). Upon binding the ZZ domain of the autophagic cargo receptor SQSTM1/p62 (sequestosome 1), these chemicals induced the biogenesis and recruitment of autophagic membranes to intracellular bacteria via SQSTM1, leading to lysosomal degradation. The antimicrobial efficacy was independent of rapamycin-modulated core autophagic pathways and synergistic with the reduced production of inflammatory cytokines. In mice, these drugs exhibited antimicrobial efficacy for S. Typhimurium, Bacillus Calmette–Guérin (BCG), and Mtb as well as multidrug-resistant Mtb and inhibited the production of inflammatory cytokines. This dual mode of action in xenophagy and inflammation significantly protected mice from inflammatory lesions in the lungs and other tissues caused by all the tested bacterial strains. Our results suggest that the N-degron pathway provides a therapeutic target in host-directed therapeutics for a broad range of drug-resistant intracellular pathogens. Abbreviations: ATG: autophagy-related gene; BCG: Bacillus Calmette–Guérin; BMDMs: bone marrow-derived macrophages; CALCOCO2/NDP52: calcium binding and coiled-coil domain 2; CFUs: colony-forming units; CXCL: C-X-C motif chemokine ligand; EGFP: enhanced green fluorescent protein; IL1B/IL-1β: interleukin 1 beta; IL6: interleukin 6; LIR: MAP1LC3/LC3-interacting region; MAP1LC3/LC3: microtubule associated protein 1 light chain 3; Mtb: Mycobacterium tuberculosis; MTOR: mechanistic target of rapamycin kinase; NBR1: NBR1 autophagy cargo receptor; OPTN: optineurin; PB1: Phox and Bem1; SQSTM1/p62: sequestosome 1; S. Typhimurium: Salmonella enterica serovar Typhimurium; TAX1BP1: Tax1 binding protein 1; TNF: tumor necrosis factor; UBA: ubiquitin-associated.

Published

2022

5. The Cys-N-degron pathway modulates pexophagy through the N-terminal oxidation and arginylation of ACAD10

Author

Sang Mi Shim, Ha Rim Choi, Soon Chul Kwon, Hye Yeon Kim, Ki Woon Sung, Eui Jung Jung, Su Ran Mun, Tae Hyun Bae, Dong Hyun Kim, Yeon Sung Son, Chan Hoon Jung, Jihoon Lee, Min Jae Lee, Joo-Won Park, and Yong Tae Kwon

Subjects

Cell Biology, Molecular Biology

Abstract

In the N-degron pathway, N-recognins recognize cognate substrates for degradation via the ubiquitin (Ub)-proteasome system (UPS) or the autophagy-lysosome system (hereafter autophagy). We have recently shown that the autophagy receptor SQSTM1/p62 (sequestosome 1) is an N-recognin that binds the N-terminal arginine (Nt-Arg) as an N-degron to modulate autophagic proteolysis. Here, we show that the N-degron pathway mediates pexophagy, in which damaged peroxisomal fragments are degraded by autophagy under normal and oxidative stress conditions. This degradative process initiates when the Nt-Cys of ACAD10 (acyl-CoA dehydrogenase family, member 10), a receptor in pexophagy, is oxidized into Cys sulfinic (CysO2) or sulfonic acid (CysO3) by ADO (2-aminoethanethiol (cysteamine) dioxygenase). Under oxidative stress, the Nt-Cys of ACAD10 is chemically oxidized by reactive oxygen species (ROS). The oxidized Nt-Cys2 is arginylated by ATE1-encoded R-transferases, generating the RCOX N-degron. RCOX-ACAD10 marks the site of pexophagy via the interaction with PEX5 and binds the ZZ domain of SQSTM1/p62, recruiting LC3+-autophagic membranes. In mice, knockout of either Ate1 responsible for Nt-arginylation or Sqstm1/p62 leads to increased levels of peroxisomes. In the cells from patients with peroxisome biogenesis disorders (PBDs), characterized by peroxisomal loss due to uncontrolled pexophagy, inhibition of either ATE1 or SQSTM1/p62 was sufficient to recover the level of peroxisomes. Our results demonstrate that the Cys-N-degron pathway generates an N-degron that regulates the removal of damaged peroxisomal membranes along with their contents. We suggest that tannic acid, a commercially available drug on the market, has a potential to treat PBDs through its activity to inhibit ATE1 R-transferases. Abbreviations: ACAA1, acetyl-Coenzyme A acyltransferase 1; ACAD, acyl-Coenzyme A dehydrogenase; ADO, 2-aminoethanethiol (cysteamine) dioxygenase; ATE1, arginyltransferase 1; CDO1, cysteine dioxygenase type 1; ER, endoplasmic reticulum; LIR, LC3-interacting region; MOXD1, monooxygenase, DBH-like 1; NAC, N-acetyl-cysteine; Nt-Arg, N-terminal arginine; Nt-Cys, N-terminal cysteine; PB1, Phox and Bem1p; PBD, peroxisome biogenesis disorder; PCO, plant cysteine oxidase; PDI, protein disulfide isomerase; PTS, peroxisomal targeting signal; R-COX, Nt-Arg-CysOX; RNS, reactive nitrogen species; ROS, reactive oxygen species; SNP, sodium nitroprusside; UBA, ubiquitin-associated; UPS, ubiquitinproteasome system.

Published

2022