Your search keyword '"Yu, Jungeun"' showing total 32 results

1. NOTCH2 promotes osteoclast maturation and metabolism and modulates the transcriptome profile during osteoclastogenesis

Author

Canalis, Ernesto, Schilling, Lauren, Yu, Jungeun, and Denker, Emily

Published

2024

2. NOTCH2 sensitizes the chondrocyte to the inflammatory response of tumor necrosis factor α

Author

Canalis, Ernesto, Yu, Jungeun, Singh, Vijender, Mocarska, Magda, and Schilling, Lauren

Published

2023

3. Notch and the regulation of osteoclast differentiation and function

Author

Yu, Jungeun and Canalis, Ernesto

Published

2020

4. Cbl-PI3K interaction regulates Cathepsin K secretion in osteoclasts

Author

Yu, Jungeun, Adapala, Naga Suresh, Doherty, Laura, and Sanjay, Archana

Published

2019

5. Induction of the Hajdu-Cheney Syndrome Mutation in CD19 B Cells in Mice Alters B-Cell Allocation but Not Skeletal Homeostasis

Author

Yu, Jungeun, Zanotti, Stefano, Schilling, Lauren, Schoenherr, Chris, Economides, Aris N., Sanjay, Archana, and Canalis, Ernesto

Published

2018

6. Loss of Cbl-PI3K interaction modulates the periosteal response to fracture by enhancing osteogenic commitment and differentiation

Author

Scanlon, Vanessa, Walia, Bhavita, Yu, Jungeun, Hansen, Marc, Drissi, Hicham, Maye, Peter, and Sanjay, Archana

Published

2017

7. Use of antisense oligonucleotides to target Notch3 in skeletal cells

Author

Canalis, Ernesto, primary, Carrer, Michele, additional, Eller, Tabitha, additional, Schilling, Lauren, additional, and Yu, Jungeun, additional

Published

2022

8. 1,3-Dibenzyl-5-Fluorouracil Prevents Ovariectomy-Induced Bone Loss by Suppressing Osteoclast Differentiation

Author

Jeon, Hyoeun, primary, Yu, Jungeun, additional, Hwang, Jung Me, additional, Park, Hye-Won, additional, Yu, Jiyeon, additional, Lee, Zee-Won, additional, Kim, Taesoo, additional, and Rho, Jaerang, additional

Published

2022

9. Hairy and enhancer of split 1 is a primary effector of NOTCH2 signaling and induces osteoclast differentiation and function

Author

Yu, Jungeun, primary, Schilling, Lauren, additional, Eller, Tabitha, additional, and Canalis, Ernesto, additional

Published

2021

10. D-chiro-inositol Negatively Regulates the Formation of Multinucleated Osteoclasts by Down-Regulating NFATc1

Author

Yu, Jungeun, Choi, Seunga, Park, Eui-Soon, Shin, Bongjin, Yu, Jiyeon, Lee, Seoung Hoon, Takami, Masamichi, Kang, Jong Soon, Meong, Hyungun, and Rho, Jaerang

Published

2012

11. T-Cell Death Associated Gene 51 Is a Novel Negative Regulator of PPARγ That Inhibits PPARγRXRα Heterodimer Formation in Adipogenesis

Author

Kim, Sumi, primary, Lee, Nari, additional, Park, Eui-Soon, additional, Yun, Hyeongseok, additional, Ha, Tae-Uk, additional, Jeon, Hyoeun, additional, Yu, Jiyeon, additional, Choi, Seunga, additional, Shin, Bongjin, additional, Yu, Jungeun, additional, Rhee, Sang Dal, additional, Choi, Yongwon, additional, and Rho, Jaerang, additional

Published

2021

12. Activation of Notch3 in osteoblasts/osteocytes causes compartment-specific changes in bone remodeling

Author

Canalis, Ernesto, primary, Zanotti, Stefano, additional, Schilling, Lauren, additional, Eller, Tabitha, additional, and Yu, Jungeun, additional

Published

2021

13. Nuclear factor of activated T cells 1 and 2 are required for vertebral homeostasis

Author

Canalis, Ernesto, primary, Schilling, Lauren, additional, Eller, Tabitha, additional, and Yu, Jungeun, additional

Published

2020

14. Antisense oligonucleotides targeting Notch2 ameliorate the osteopenic phenotype in a mouse model of Hajdu-Cheney syndrome

Author

Canalis, Ernesto, primary, Grossman, Tamar R., additional, Carrer, Michele, additional, Schilling, Lauren, additional, and Yu, Jungeun, additional

Published

2020

15. A PDGFRβ-PI3K signaling axis mediates periosteal cell activation during fracture healing

Author

Doherty, Laura, primary, Yu, Jungeun, additional, Wang, Xi, additional, Hankenson, Kurt D., additional, Kalajzic, Ivo, additional, and Sanjay, Archana, additional

Published

2019

16. The Hajdu Cheney mutation sensitizes mice to the osteolytic actions of tumor necrosis factor α

Author

Yu, Jungeun, primary and Canalis, Ernesto, additional

Published

2019

17. TDAG51 is a crucial regulator of maternal care and depressive-like behavior after parturition

Author

Yun, Hyeongseok, primary, Park, Eui-Soon, additional, Choi, Seunga, additional, Shin, Bongjin, additional, Yu, Jungeun, additional, Yu, Jiyeon, additional, Amarasekara, Dulshara Sachini, additional, Kim, Sumi, additional, Lee, Nari, additional, Choi, Jong-Soon, additional, Choi, Yongwon, additional, and Rho, Jaerang, additional

Published

2019

18. An antibody to Notch3 reverses the skeletal phenotype of lateral meningocele syndrome in male mice

Author

Yu, Jungeun, primary, Siebel, Christian W., additional, Schilling, Lauren, additional, and Canalis, Ernesto, additional

Published

2019

19. PDGF Modulates BMP2-Induced Osteogenesis in Periosteal Progenitor Cells

Author

Wang, Xi, primary, Matthews, Brya G, additional, Yu, Jungeun, additional, Novak, Sanja, additional, Grcevic, Danka, additional, Sanjay, Archana, additional, and Kalajzic, Ivo, additional

Published

2019

20. An antibody to Notch3 reverses the skeletal phenotype of lateral meningocele syndrome in male mice.

Author

Yu, Jungeun, Siebel, Christian W., Schilling, Lauren, and Canalis, Ernesto

Subjects

*NOTCH genes, *CANCELLOUS bone, *GLUTAMIC acid, *SKELETAL abnormalities, *IMMUNOGLOBULINS, *MESSENGER RNA, *OSTEOBLASTS

Abstract

Lateral meningocele syndrome (LMS), a genetic disorder characterized by meningoceles and skeletal abnormalities, is associated with NOTCH3 mutations. We created a mouse model of LMS (Notch3tm1.1Ecan) by introducing a tandem termination codon in the Notch3 locus upstream of the proline (P), glutamic acid (E), serine (S) and threonine (T) domain. Microcomputed tomography demonstrated that Notch3tm1.1Ecan mice exhibit osteopenia. The cancellous bone osteopenia was no longer observed after the intraperitoneal administration of antibodies directed to the negative regulatory region (NRR) of Notch3. The anti‐Notch3 NRR antibody suppressed the expression of Hes1, Hey1, and Hey2 (Notch target genes), and decreased Tnfsf11 (receptor activator of NF Kappa B ligand) messenger RNA in Notch3tm1.1Ecan osteoblast (OB) cultures. Bone marrow‐derived macrophages (BMMs) from Notch3tm1.1Ecan mutants exhibited enhanced osteoclastogenesis in culture, and this was increased in cocultures with Notch3tm1.1Ecan OB. Osteoclastogenesis was suppressed by anti‐Notch3 NRR antibodies in Notch3tm1.1Ecan OB/BMM cocultures. In conclusion, the cancellous bone osteopenia of Notch3tm1.1Ecan mutants is reversed by anti‐Notch3 NRR antibodies. [ABSTRACT FROM AUTHOR]

Published

2020

21. The lateral meningocele syndrome mutation causes marked osteopenia in mice

Author

Canalis, Ernesto, primary, Yu, Jungeun, additional, Schilling, Lauren, additional, Yee, Siu-Pok, additional, and Zanotti, Stefano, additional

Published

2018

22. Nuclear factor of activated T cells 2 is required for osteoclast differentiation and function in vitro but not in vivo

Author

Yu, Jungeun, primary, Zanotti, Stefano, additional, Schilling, Lauren, additional, and Canalis, Ernesto, additional

Published

2018

23. Glucocorticoids inhibit notch target gene expression in osteoblasts

Author

Zanotti, Stefano, primary, Yu, Jungeun, additional, Adhikari, Suyash, additional, and Canalis, Ernesto, additional

Published

2018

24. The Hajdu Cheney Mutation Is a Determinant of B-Cell Allocation of the Splenic Marginal Zone

Author

Yu, Jungeun, primary, Zanotti, Stefano, additional, Walia, Bhavita, additional, Jellison, Evan, additional, Sanjay, Archana, additional, and Canalis, Ernesto, additional

Published

2018

25. Sustained Notch2 signaling in osteoblasts, but not in osteoclasts, is linked to osteopenia in a mouse model of Hajdu-Cheney syndrome

Author

Zanotti, Stefano, primary, Yu, Jungeun, additional, Sanjay, Archana, additional, Schilling, Lauren, additional, Schoenherr, Chris, additional, Economides, Aris N., additional, and Canalis, Ernesto, additional

Published

2017

26. An Antibody to Notch2 Reverses the Osteopenic Phenotype of Hajdu-Cheney Mutant Male Mice

Author

Canalis, Ernesto, primary, Sanjay, Archana, additional, Yu, Jungeun, additional, and Zanotti, Stefano, additional

Published

2017

27. Interaction of Tumor Necrosis Factor Receptor-associated Factor 6 (TRAF6) and Vav3 in the Receptor Activator of Nuclear Factor κB (RANK) Signaling Complex Enhances Osteoclastogenesis

Author

Yu, Jiyeon, primary, Yun, Hyeongseok, additional, Shin, Bongjin, additional, Kim, Yongjin, additional, Park, Eui-Soon, additional, Choi, Seunga, additional, Yu, Jungeun, additional, Amarasekara, Dulshara Sachini, additional, Kim, Sumi, additional, Inoue, Jun-ichiro, additional, Walsh, Matthew C., additional, Choi, Yongwon, additional, Takami, Masamichi, additional, and Rho, Jaerang, additional

Published

2016

28. Increased periosteal expansion, Osterix expression and osteogenic potential upon bone injury during perturbed PI3K signaling

Author

Walia, Bhavita, primary, Scanlon, Vanessa, additional, Yu, Jungeun, additional, Maye, Peter, additional, Drissi, Hicham, additional, and Sanjay, Archana, additional

Published

2016

29. Tumor Necrosis Factor (TNF) Receptor-associated Factor (TRAF)-interacting Protein (TRIP) Negatively Regulates the TRAF2 Ubiquitin-dependent Pathway by Suppressing the TRAF2-Sphingosine 1-Phosphate (S1P) Interaction

Author

Park, Eui-Soon, primary, Choi, Seunga, additional, Shin, Bongjin, additional, Yu, Jungeun, additional, Yu, Jiyeon, additional, Hwang, Jung-Me, additional, Yun, Hyeongseok, additional, Chung, Young-Ho, additional, Choi, Jong-Soon, additional, Choi, Yongwon, additional, and Rho, Jaerang, additional

Published

2015

30. Secretion of a Truncated Osteopetrosis-associated Transmembrane Protein 1 (OSTM1) Mutant Inhibits Osteoclastogenesis through Down-regulation of the B Lymphocyte-induced Maturation Protein 1 (BLIMP1)-Nuclear Factor of Activated T Cells c1 (NFATc1) Axis

Author

Shin, Bongjin, primary, Yu, Jungeun, additional, Park, Eui-Soon, additional, Choi, Seunga, additional, Yu, Jiyeon, additional, Hwang, Jung Me, additional, Yun, Hyeongseok, additional, Chung, Young-Ho, additional, Hong, Kwan Soo, additional, Choi, Jong-Soon, additional, Takami, Masamichi, additional, and Rho, Jaerang, additional

Published

2014

31. Protein arginine methyltransferase 1 regulates herpes simplex virus replication through ICP27 RGG-box methylation

Author

Yu, Jungeun, primary, Shin, Bongjin, additional, Park, Eui-Soon, additional, Yang, Sujeong, additional, Choi, Seunga, additional, Kang, Misun, additional, and Rho, Jaerang, additional

Published

2010

32. T-Cell Death Associated Gene 51 Is a Novel Negative Regulator of PPARγ That Inhibits PPARγ-RXRα Heterodimer Formation in Adipogenesis

Author

Kim S, Lee N, Park ES, Yun H, Ha TU, Jeon H, Yu J, Choi S, Shin B, Yu J, Rhee SD, Choi Y, and Rho J

Subjects

3T3-L1 Cells, Adipocytes cytology, Adipocytes metabolism, Animals, Cell Death, Fatty Acid-Binding Proteins genetics, Fatty Acid-Binding Proteins metabolism, Mice, Promoter Regions, Genetic genetics, Protein Binding, Transcription Factors metabolism, Adipogenesis, PPAR gamma metabolism, Protein Multimerization, Retinoid X Receptor alpha metabolism, T-Lymphocytes cytology, T-Lymphocytes metabolism, Transcription Factors genetics

Abstract

The nuclear receptor peroxisome proliferator-activated receptor γ (PPARγ) is the master transcriptional regulator in adipogenesis. PPARγ forms a heterodimer with another nuclear receptor, retinoid X receptor (RXR), to form an active transcriptional complex, and their transcriptional activity is tightly regulated by the association with either coactivators or corepressors. In this study, we identified T-cell death-associated gene 51 (TDAG51) as a novel corepressor of PPARγ-mediated transcriptional regulation. We showed that TDAG51 expression is abundantly maintained in the early stage of adipogenic differentiation. Forced expression of TDAG51 inhibited adipocyte differentiation in 3T3-L1 cells. We found that TDAG51 physically interacts with PPARγ in a ligand-independent manner. In deletion mutant analyses, large portions of the TDAG51 domains, including the pleckstrin homology-like, glutamine repeat and proline-glutamine repeat domains but not the proline-histidine repeat domain, are involved in the interaction with the region between residues 140 and 506, including the DNA binding domain, hinge, ligand binding domain and activation function-2 domain, in PPARγ. The heterodimer formation of PPARγ-RXRα was competitively inhibited in a ligand-independent manner by TDAG51 binding to PPARγ. Thus, our data suggest that TDAG51, which could determine adipogenic cell fate, acts as a novel negative regulator of PPARγ by blocking RXRα recruitment to the PPARγ-RXRα heterodimer complex in adipogenesis.

Published

2021