Your search keyword '"Jia-Bin Pan"' showing total 17 results

1. Enantioselective synthesis of chiral amides by carbene insertion into amide N–H bond

Author

Xuan-Ge Zhang, Zhi-Chun Yang, Jia-Bin Pan, Xiao-Hua Liu, and Qi-Lin Zhou

Subjects

Science

Abstract

Abstract Chiral amides are important structure in many natural products and pharmaceuticals, yet their efficient synthesis from simple amide feedstock remains challenge due to its weak Lewis basicity. Herein, we describe our study of the enantioselective synthesis of chiral amides by N-alkylation of primary amides taking advantage of an achiral rhodium and chiral squaramide co-catalyzed carbene N–H insertion reaction. This method features mild condition, rapid reaction rate (in all cases 1 min) and a wide substrate scope with high yield and excellent enantioselectivity. Further product transformations show the synthetic potential of this reaction. Mechanistic studies reveal that the non-covalent interactions between the catalyst and reaction intermediate play a critical role in enantiocontrol.

Published

2024

2. Jdp2 is a spatiotemporal transcriptional activator of the AhR via the Nrf2 gene battery

Author

Kenly Wuputra, Ming-Ho Tsai, Kohsuke Kato, Chia-Chen Ku, Jia-Bin Pan, Ya-Han Yang, Shigeo Saito, Chun-Chieh Wu, Ying-Chu Lin, Kuang-Hung Cheng, Kung-Kai Kuo, Michiya Noguchi, Yukio Nakamura, Tohru Yoshioka, Deng-Chyang Wu, Chang-Shen Lin, and Kazunari K. Yokoyama

Subjects

Antioxidation, Aryl hydrocarbon receptor, Dioxin responsive element, Nuclear factor (erythroid-derived 2)-like 2 transcription factor, Jun dimerization protein 2, Oxidative stress, Pathology, RB1-214

Abstract

Abstract Background Crosstalk between the aryl hydrocarbon receptor (AhR) and nuclear factor (erythroid-derived 2)-like 2 (Nrf2) signaling is called the “AhR–Nrf2 gene battery”, which works synergistically in detoxification to support cell survival. Nrf2-dependent phase II gene promoters are controlled by coordinated recruitment of the AhR to adjacent dioxin responsive element (DRE) and Nrf2 recruitment to the antioxidative response element (ARE). The molecular interaction between AhR and Nrf2 members, and the regulation of each target, including phase I and II gene complexes, and their mediators are poorly understood. Methods Knockdown and forced expression of AhR–Nrf2 battery members were used to examine the molecular interactions between the AhR–Nrf2 axis and AhR promoter activation. Sequential immunoprecipitation, chromatin immunoprecipitation, and histology were used to identify each protein complex recruited to their respective cis-elements in the AhR promoter. Actin fiber distribution, cell spreading, and invasion were examined to identify functional differences in the AhR–Jdp2 axis between wild-type and Jdp2 knockout cells. The possible tumorigenic role of Jdp2 in the AhR–Nrf2 axis was examined in mutant Kras-Trp53-driven pancreatic tumors. Results Crosstalk between AhR and Nrf2 was evident at the transcriptional level. The AhR promoter was activated by phase I ligands such as 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) through the AhR–Jdp2–Nrf2 axis in a time- and spatial transcription-dependent manner. Jdp2 was a bifunctional activator of DRE- and ARE-mediated transcription in response to TCDD. After TCDD exposure, Jdp2 activated the AhR promoter at the DRE and then moved to the ARE where it activated the promoter to increase reactive oxygen species (ROS)-mediated functions such as cell spreading and invasion in normal cells, and cancer regression in mutant Kras-Trp53-driven pancreatic tumor cells. Conclusions Jdp2 plays a critical role in AhR promoter activation through the AhR–Jdp2–Nrf2 axis in a spatiotemporal manner. The AhR functions to maintain ROS balance and cell spreading, invasion, and cancer regression in a mouse model of mutant Kras–Trp53 pancreatic cancer. These findings provide new insights into the roles of Jdp2 in the homeostatic regulation of oxidative stress and in the antioxidation response in detoxification, inflammation, and cancer progression.

Published

2023

3. Deletion of Jdp2 enhances Slc7a11 expression in Atoh-1 positive cerebellum granule cell progenitors in vivo

Author

Chia-Chen Ku, Kenly Wuputra, Kohsuke Kato, Jia-Bin Pan, Chia-Pei Li, Ming-Ho Tsai, Michiya Noguchi, Yukio Nakamura, Chung-Jung Liu, Te-Fu Chan, Ming-Feng Hou, Shigeharu Wakana, Yang-Chang Wu, Chang-Shen Lin, Deng-Chyang Wu, and Kazunari K. Yokoyama

Subjects

Antioxidation, Cerebellum, Granule cells, Jun dimerization protein 2 (Jdp2), Reactive oxygen species (ROS), Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract Background The cerebellum is the sensitive region of the brain to developmental abnormalities related to the effects of oxidative stresses. Abnormal cerebellar lobe formation, found in Jun dimerization protein 2 (Jdp2)-knockout (KO) mice, is related to increased antioxidant formation and a reduction in apoptotic cell death in granule cell progenitors (GCPs). Here, we aim that Jdp2 plays a critical role of cerebellar development which is affected by the ROS regulation and redox control. Objective Jdp2-promoter-Cre transgenic mouse displayed a positive signal in the cerebellum, especially within granule cells. Jdp2-KO mice exhibited impaired development of the cerebellum compared with wild-type (WT) mice. The antioxidation controlled gene, such as cystine-glutamate transporter Slc7a11, might be critical to regulate the redox homeostasis and the development of the cerebellum. Methods We generated the Jdp2-promoter-Cre mice and Jdp2-KO mice to examine the levels of Slc7a11, ROS levels and the expressions of antioxidation related genes were examined in the mouse cerebellum using the immunohistochemistry. Results The cerebellum of Jdp2-KO mice displayed expression of the cystine-glutamate transporter Slc7a11, within the internal granule layer at postnatal day 6; in contrast, the WT cerebellum mainly displayed Sla7a11 expression in the external granule layer. Moreover, development of the cerebellar lobes in Jdp2-KO mice was altered compared with WT mice. Expression of Slc7a11, Nrf2, and p21Cip1 was higher in the cerebellum of Jdp2-KO mice than in WT mice. Conclusion Jdp2 is a critical regulator of Slc7a11 transporter during the antioxidation response, which might control the growth, apoptosis, and differentiation of GCPs in the cerebellar lobes. These observations are consistent with our previous study in vitro.

Published

2021

4. Redox control in the pathophysiology of influenza virus infection

Author

Ker-Kong Chen, Moeko Minakuchi, Kenly Wuputra, Chia-Chen Ku, Jia-Bin Pan, Kung-Kai Kuo, Ying-Chu Lin, Shigeo Saito, Chang-Shen Lin, and Kazunari K. Yokoyama

Subjects

Antioxidation, Aryl hydrocarbon receptor, Cellular oxidation, Nuclear factor E2-related factor 2, Reactive oxygen species, Microbiology, QR1-502

Abstract

Abstract Triggered in response to external and internal ligands in cells and animals, redox homeostasis is transmitted via signal molecules involved in defense redox mechanisms through networks of cell proliferation, differentiation, intracellular detoxification, bacterial infection, and immune reactions. Cellular oxidation is not necessarily harmful per se, but its effects depend on the balance between the peroxidation and antioxidation cascades, which can vary according to the stimulus and serve to maintain oxygen homeostasis. The reactive oxygen species (ROS) that are generated during influenza virus (IV) infection have critical effects on both the virus and host cells. In this review, we outline the link between viral infection and redox control using IV infection as an example. We discuss the current state of knowledge on the molecular relationship between cellular oxidation mediated by ROS accumulation and the diversity of IV infection. We also summarize the potential anti-IV agents available currently that act by targeting redox biology/pathophysiology.

Published

2020

5. Generation of Human Stomach Cancer iPSC-Derived Organoids Induced by Helicobacter pylori Infection and Their Application to Gastric Cancer Research

Author

Chia-Chen Ku, Kenly Wuputra, Jia-Bin Pan, Chia-Pei Li, Chung-Jung Liu, Yi-Chang Liu, Shigeo Saito, Te-Fu Chan, Chang-Shen Lin, Deng-Chyang Wu, and Kazunari K. Yokoyama

Subjects

stomach antral stem cells, stomach corpus stem cells, Helicobacter pylori, organoids, stem cell niches, Cytology, QH573-671

Abstract

There is considerable cellular diversity in the human stomach, which has helped to clarify cell plasticity in normal development and tumorigenesis. Thus, the stomach is an interesting model for understanding cellular plasticity and for developing prospective anticancer therapeutic agents. However, many questions remain regarding the development of cancers in vivo and in vitro in two- or three-dimensional (2D/3D) cultures, as well as the role of Helicobacter pylori (H. p.) infection. Here, we focus on the characteristics of cancer stem cells and their derived 3D organoids in culture, including the formation of stem cell niches. We define the conditions required for such organoid culture in vitro and examine the ability of such models for testing the use of anticancer agents. We also summarize the signaling cascades and the specific markers of stomach-cancer-derived organoids induced by H. p. infection, and their stem cell niches.

Published

2022

6. Enantioselective Synthesis of Chiral Amides by Phosphoric Acid-Catalyzed Asymmetric Wolff Rearrangement

Author

Jia-Bin Pan, Zhi-Chun Yang, Xuan-Ge Zhang, Mao-Lin Li, and Qi-Lin Zhou

Abstract

The enantioselective addition of potent nucleophilic reagents to ketene compounds poses challenges due to the presence of significant background reactions, along with simultaneous stereoselectivity and enantioselectivity issues in the reaction process. We present a method for enantioselective amination of ketenes employing α-aryl-α-diazoketones as ketene precursors and phosphoric acids as catalysts. Upon exposure to visible light, diazoketones undergo Wolff rearrangement to gradually generate ketenes. Subsequently, the phosphoric acid not only accelerates capture of ketenes by amines, forming a singular configuration of aminoenol intermediates, but also promotes the enantioselective proton transfer of the intermediates to yield product. Mechanism studies elucidate the reaction pathways and explain how the catalysts expedite this transformation and control enantioselectivity.

Published

2023

7. Enantioselective synthesis of amino acids from ammonia

Author

Mao-Lin Li, Jia-Bin Pan, and Qi-Lin Zhou

Subjects

Process Chemistry and Technology, Bioengineering, Biochemistry, Catalysis

Published

2022

8. Independent Signaling of Hepatoma Derived Growth Factor and Tumor Necrosis Factor-Alpha in Human Gastric Cancer Organoids Infected by Helicobacter pylori

Author

Kenly Wuputra, Chia-Chen Ku, Jia-Bin Pan, Chung-Jung Liu, Kohsuke Kato, Ying-Chu Lin, Yi-Chang Liu, Chang-Shen Lin, Michael Hsiao, Ming-Hong Tai, Inn-Wen Chong, Huang-Ming Hu, Chao-Hung Kuo, Deng-Chyang Wu, and Kazunari K. Yokoyama

Subjects

Inorganic Chemistry, Organic Chemistry, Helicobacter pylori, hepatoma-derived growth factor, invasion activity, gastric cancer organoids, tumor necrosis factor α, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

We prepared three-dimensional (3-D) organoids of human stomach cancers and examined the correlation between the tumorigenicity and cytotoxicity of Helicobacter pylori (H. pylori). In addition, the effects of hepatoma-derived growth factor (HDGF) and tumor necrosis factor (TNFα) on the growth and invasion activity of H. pylori-infected gastric cancer organoids were examined. Cytotoxin-associated gene A (CagA)-green fluorescence protein (GFP)-labeled H. pylori was used to trace the infection in gastric organoids. The cytotoxicity of Cag encoded toxins from different species of H. pylori did not affect the proliferation of each H. pylori-infected cancer organoid. To clarify the role of HDGF and TNFα secreted from H. pylori-infected cancer organoids, we prepared recombinant HDGF and TNFα and measured the cytotoxicity and invasion of gastric cancer organoids. HDGF controlled the growth of each organoid in a species-specific manner of H. pylori, but TNFα decreased the cell viability in H. pylori-infected cancer organoids. Furthermore, HDGF controlled the invasion activity of H. pylori-infected cancer organoid in a species-dependent manner. However, TNFα decreased the invasion activities of most organoids. We found different signaling of cytotoxicity and invasion of human gastric organoids in response to HDGF and TNFα during infection by H. pylori. Recombinant HDGF and TNFα inhibited the development and invasion of H. pylori-infected gastric cancer differently. Thus, we propose that HDGF and TNFα are independent signals for development of H. pylori-infected gastric cancer. The signaling of growth factors in 3-D organoid culture systems is different from those in two-dimensional cancer cells.

Published

2023

9. A Spiro Phosphamide Catalyzed Enantioselective Proton Transfer of Ylides in a Free Carbene Insertion into N−H Bonds

Author

Jia‐Bin Pan, Xuan‐Ge Zhang, Yi‐Fan Shi, Ai‐Cui Han, Yu‐Jia Chen, Jing Ouyang, Mao‐Lin Li, and Qi‐Lin Zhou

Subjects

General Medicine, General Chemistry, Catalysis

Published

2023

10. Dimethyl sulfoxide stimulates the AhR-Jdp2 axis to control ROS accumulation in mouse embryonic fibroblasts

Author

Hua-Ling Chen, Ying-Chu Lin, Shotaro Kishikawa, Ya-Han Yang, Shau-Ku Huang, Te-Fu Chan, Jia-Bin Pan, Chia-Chen Ku, Kohsuke Kato, Deng-Chyang Wu, Kung-Kai Kuo, Michiya Noguchi, Chung-Jung Liu, Ming-Feng Hou, Ming-Ho Tsai, Yukio Nakamura, Kenly Wuputra, Kazunari K. Yokoyama, Chang-Shen Lin, and Koji Nakade

Subjects

0301 basic medicine, Polychlorinated Dibenzodioxins, Aryl hydrocarbon receptor nuclear translocator, NF-E2-Related Factor 2, Immunoprecipitation, Health, Toxicology and Mutagenesis, Ligands, Toxicology, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Transcription (biology), Animals, Dimethyl Sulfoxide, Transcription factor, biology, Chemistry, Dimethyl sulfoxide, Cell Biology, Fibroblasts, Aryl hydrocarbon receptor, Cell biology, 030104 developmental biology, Receptors, Aryl Hydrocarbon, 030220 oncology & carcinogenesis, Jun dimerization protein, biology.protein, Reactive Oxygen Species, Chromatin immunoprecipitation

Abstract

The aryl hydrocarbon receptor (AhR) is a ligand-binding protein that responds to environmental aromatic hydrocarbons and stimulates the transcription of downstream phase I enzyme–related genes by binding the cis element of dioxin-responsive elements (DREs)/xenobiotic-responsive elements. Dimethyl sulfoxide (DMSO) is a well-known organic solvent that is often used to dissolve phase I reagents in toxicology and oxidative stress research experiments. In the current study, we discovered that 0.1% DMSO significantly induced the activation of the AhR promoter via DREs and produced reactive oxygen species, which induced apoptosis in mouse embryonic fibroblasts (MEFs). Moreover, Jun dimerization protein 2 (Jdp2) was found to be required for activation of the AhR promoter in response to DMSO. Coimmunoprecipitation and chromatin immunoprecipitation studies demonstrated that the phase I–dependent transcription factors, AhR and the AhR nuclear translocator, and phase II–dependent transcription factors such as nuclear factor (erythroid-derived 2)–like 2 (Nrf2) integrated into DRE sites together with Jdp2 to form an activation complex to increase AhR promoter activity in response to DMSO in MEFs. Our findings provide evidence for the functional role of Jdp2 in controlling the AhR gene via Nrf2 and provide insights into how Jdp2 contributes to the regulation of ROS production and the cell spreading and apoptosis produced by the ligand DMSO in MEFs. Graphical abstract

Published

2021

11. Carboxyl Group-Directed Iridium-Catalyzed Enantioselective Hydrogenation of Aliphatic γ-Ketoacids

Author

Qi-Lin Zhou, Yao Li, Song Song, Shou-Fei Zhu, Mao-Lin Li, Jia-Bin Pan, and Yi-Hao Li

Subjects

010405 organic chemistry, Chemistry, Asymmetric hydrogenation, Aromatic ketones, Enantioselective synthesis, chemistry.chemical_element, General Chemistry, 010402 general chemistry, 01 natural sciences, Medicinal chemistry, Catalysis, 0104 chemical sciences, Group (periodic table), Iridium

Abstract

Although the transition metal-catalyzed asymmetric hydrogenation of aromatic ketones has been extensively explored, the enantioselective hydrogenation of aliphatic ketones remains a challenge becau...

Published

2020

12. Stem Cell Biomarkers and Tumorigenesis in Gastric Cancer

Author

Kenly Wuputra, Chia-Chen Ku, Jia-Bin Pan, Chung-Jung Liu, Yi-Chang Liu, Shigeo Saito, Kohsuke Kato, Ying-Chu Lin, Kung-Kai Kuo, Te-Fu Chan, Inn-Wen Chong, Chang-Shen Lin, Deng-Chyang Wu, and Kazunari K. Yokoyama

Subjects

Medicine (miscellaneous)

Abstract

Stomach cancer has a high mortality, which is partially caused by an absence of suitable biomarkers to allow detection of the initiation stages of cancer progression. Thus, identification of critical biomarkers associated with gastric cancer (GC) is required to advance its clinical diagnoses and treatment. Recent studies using tracing models for lineage analysis of GC stem cells indicate that the cell fate decision of the gastric stem cells might be an important issue for stem cell plasticity. They include leucine-rich repeat-containing G-protein-coupled receptor 5 (Lgr5+), Cholecystokinin receptor 2 (Cckr2+), and axis inhibition protein 2 (Axin2+) as the stem cell markers in the antrum, Trefoil Factor 2 (TFF2+), Mist1+ stem cells, and Troy+ chief cells in the corpus. By contrast, Estrogen receptor 1 (eR1), Leucine-rich repeats and immunoglobulin-like domains 1 (Lrig1), SRY (sex determining region Y)-box 2 (Sox2), and B lymphoma Mo-MLV insertion region 1 homolog (Bmi1) are rich in both the antrum and corpus regions. These markers might help to identify the cell-lineage identity and analyze the plasticity of each stem cell population. Thus, identification of marker genes for the development of GC and its environment is critical for the clinical application of cancer stem cells in the prevention of stomach cancers.

Published

2022

13. Therapeutic Strategies Targeting Tumor Suppressor Genes in Pancreatic Cancer

Author

Ya-Han Yang, Chia-Chen Ku, Kohsuke Kato, Jia-Bin Pan, Chung-Jung Liu, Pi-Jung Hsiao, Deng-Chyang Wu, Wen-Tsan Chang, Kung-Kai Kuo, Chia-Pei Li, Shih-Chang Chuang, Kazunari K. Yokoyama, and Kenly Wuputra

Subjects

0301 basic medicine, Oncology, p53, Cancer Research, medicine.medical_specialty, Tumor suppressor gene, medicine.medical_treatment, pancreatic cancer, Review, Disease, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Pancreatic cancer, medicine, tumor suppressor gene, Stage (cooking), RC254-282, Chemotherapy, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, clinical trial, medicine.disease, BRCA1, BRCA2, Clinical trial, Radiation therapy, 030104 developmental biology, translational research, 030220 oncology & carcinogenesis, business

Abstract

Simple Summary Tumor suppressor genes are critical in the control of many biological functions. They can be classified based on their roles in proliferation, cell-cycle progression, DNA repair/damage, and crucial signaling functions, including apoptosis, autophagy, and necrosis. The absence of functional tumor suppressor genes entails a higher risk of dysfunction of cell growth, differentiation, cell death, and cancer development. Loss of function or mutations of such genes has been identified in many types of cancer, such as breast, bladder, colorectal, head and neck, lung, ovarian, uterine, and pancreatic cancers. Familial cancer syndromes, such as Li–Fraumeni syndrome, are associated with loss of TP53 function. Extensive studies have been carried out to clarify the roles of the products of these genes, as well as their mechanistic link to cancers, to identify novel targets for specific cancer types. Here, we introduce the roles of tumor suppressor gene products in pancreatic cancer development and its therapeutics for tumorigenesis prevention. Abstract The high mortality of pancreatic cancer is attributed to the insidious progression of this disease, which results in a delayed diagnosis and advanced disease stage at diagnosis. More than 35% of patients with pancreatic cancer are in stage III, whereas 50% are in stage IV at diagnosis. Thus, understanding the aggressive features of pancreatic cancer will contribute to the resolution of problems, such as its early recurrence, metastasis, and resistance to chemotherapy and radiotherapy. Therefore, new therapeutic strategies targeting tumor suppressor gene products may help prevent the progression of pancreatic cancer. In this review, we discuss several recent clinical trials of pancreatic cancer and recent studies reporting safe and effective treatment modalities for patients with advanced pancreatic cancer.

Published

2021

14. Biomarkers of Cancer Stem Cells for Experimental Research and Clinical Application

Author

Shigeo Saito, Chia-Chen Ku, Kenly Wuputra, Jia-Bin Pan, Chang-Shen Lin, Ying-Chu Lin, Deng-Chyang Wu, and Kazunari K. Yokoyama

Subjects

Medicine (miscellaneous)

Abstract

The use of biomarkers in cancer diagnosis, therapy, and prognosis has been highly effective over several decades. Studies of biomarkers in cancer patients pre- and post-treatment and during cancer progression have helped identify cancer stem cells (CSCs) and their related microenvironments. These analyses are critical for the therapeutic application of drugs and the efficient targeting and prevention of cancer progression, as well as the investigation of the mechanism of the cancer development. Biomarkers that characterize CSCs have thus been identified and correlated to diagnosis, therapy, and prognosis. However, CSCs demonstrate elevated levels of plasticity, which alters their functional phenotype and appearance by interacting with their microenvironments, in response to chemotherapy and radiotherapeutics. In turn, these changes induce different metabolic adaptations of CSCs. This article provides a review of the most frequently used CSCs and stem cell markers.

Published

2022

15. Author Correction: Jdp2-deficient granule cell progenitors in the cerebellum are resistant to ROS-mediated apoptosis through xCT/Slc7a11 activation

Author

Chia-Chen Ku, Kohsuke Kato, Kan-Hung Lee, Wen-Hsin Lin, Yan-Liang Lee, Ying-Chu Lin, Shigeo Saito, Shih-Chieh Tsai, Chang-Shen Lin, Yukio Nakamura, Richard Eckner, Kyosuke Nagata, Michiya Noguchi, Jia-Bin Pan, Deng-Chyang Wu, Hiroyuki Miyoshi, Che-Jung Kuo, Kenly Wuputra, and Kazunari K. Yokoyama

Subjects

Cerebellum, Multidisciplinary, biology, Chemistry, lcsh:R, lcsh:Medicine, SLC7A11, Granule cell, Cell biology, medicine.anatomical_structure, Apoptosis, biology.protein, medicine, lcsh:Q, Progenitor cell, lcsh:Science, Author Correction

Abstract

The Jun dimerization protein 2 (Jdp2) is expressed predominantly in granule cell progenitors (GCPs) in the cerebellum, as was shown in Jdp2-promoter-Cre transgenic mice. Cerebellum of Jdp2-knockout (KO) mice contains lower number of Atoh-1 positive GCPs than WT. Primary cultures of GCPs from Jdp2-KO mice at postnatal day 5 were more resistant to apoptosis than GCPs from wild-type mice. In Jdp2-KO GCPs, the levels of both the glutamate‒cystine exchanger Sc7a11 and glutathione were increased; by contrast, the activity of reactive oxygen species (ROS) was decreased; these changes confer resistance to ROS-mediated apoptosis. In the absence of Jdp2, a complex of the cyclin-dependent kinase inhibitor 1 (p21

Published

2020

16. Jdp2-deficient granule cell progenitors in the cerebellum are resistant to ROS-mediated apoptosis through xCT/Slc7a11 activation

Author

Che-Jung Kuo, Wen-Hsin Lin, Yukio Nakamura, Richard Eckner, Deng-Chyang Wu, Hiroyuki Miyoshi, Chang-Shen Lin, Shih-Chieh Tsai, Kan-Hung Lee, Ying-Chu Lin, Michiya Noguchi, Chia-Chen Ku, Kohsuke Kato, Kyosuke Nagata, Jia-Bin Pan, Kazunari K. Yokoyama, Yan-Liang Lee, Kenly Wuputra, and Shigeo Saito

Subjects

0301 basic medicine, Genetically modified mouse, Cerebellum, lcsh:Medicine, Apoptosis, SLC7A11, Molecular neuroscience, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, lcsh:Science, chemistry.chemical_classification, Reactive oxygen species, Multidisciplinary, biology, Kinase, lcsh:R, Granule cell, Cell biology, 030104 developmental biology, medicine.anatomical_structure, chemistry, 030220 oncology & carcinogenesis, biology.protein, Jun dimerization protein, lcsh:Q

Abstract

The Jun dimerization protein 2 (Jdp2) is expressed predominantly in granule cell progenitors (GCPs) in the cerebellum, as was shown in Jdp2-promoter-Cre transgenic mice. Cerebellum of Jdp2-knockout (KO) mice contains lower number of Atoh-1 positive GCPs than WT. Primary cultures of GCPs from Jdp2-KO mice at postnatal day 5 were more resistant to apoptosis than GCPs from wild-type mice. In Jdp2-KO GCPs, the levels of both the glutamate‒cystine exchanger Sc7a11 and glutathione were increased; by contrast, the activity of reactive oxygen species (ROS) was decreased; these changes confer resistance to ROS-mediated apoptosis. In the absence of Jdp2, a complex of the cyclin-dependent kinase inhibitor 1 (p21Cip1) and Nrf2 bound to antioxidant response elements of the Slc7a11 promoter and provide redox control to block ROS-mediated apoptosis. These findings suggest that an interplay between Jdp2, Nrf2, and p21Cip1 regulates the GCP apoptosis, which is one of critical events for normal development of the cerebellum.

Published

2020

17. Redox control in the pathophysiology of influenza virus infection

Author

Ying-Chu Lin, Chia-Chen Ku, Ker-Kong Chen, Kenly Wuputra, Kazunari K. Yokoyama, Kung-Kai Kuo, Jia-Bin Pan, Shigeo Saito, Chang-Shen Lin, and Moeko Minakuchi

Subjects

Microbiology (medical), lcsh:QR1-502, Review, Biology, Microbiology, Redox, Antiviral Agents, Virus, lcsh:Microbiology, 03 medical and health sciences, 0302 clinical medicine, Orthomyxoviridae Infections, Oxygen homeostasis, Influenza, Human, Animals, Homeostasis, Humans, Aryl hydrocarbon receptor, Nuclear factor E2-related factor 2, 030304 developmental biology, Cell Proliferation, chemistry.chemical_classification, 0303 health sciences, Reactive oxygen species, Cell growth, Cell Differentiation, Pathophysiology, Cell biology, chemistry, Influenza A virus, 030220 oncology & carcinogenesis, biology.protein, Antioxidation, Oxidation-Reduction, Intracellular, Cellular oxidation, Signal Transduction

Abstract

Triggered in response to external and internal ligands in cells and animals, redox homeostasis is transmitted via signal molecules involved in defense redox mechanisms through networks of cell proliferation, differentiation, intracellular detoxification, bacterial infection, and immune reactions. Cellular oxidation is not necessarily harmful per se, but its effects depend on the balance between the peroxidation and antioxidation cascades, which can vary according to the stimulus and serve to maintain oxygen homeostasis. The reactive oxygen species (ROS) that are generated during influenza virus (IV) infection have critical effects on both the virus and host cells. In this review, we outline the link between viral infection and redox control using IV infection as an example. We discuss the current state of knowledge on the molecular relationship between cellular oxidation mediated by ROS accumulation and the diversity of IV infection. We also summarize the potential anti-IV agents available currently that act by targeting redox biology/pathophysiology.

Published

2020