Your search keyword '"Yu, Jungeun"' showing total 4 results

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

Author

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

Subjects

T cells, MESENCHYMAL stem cells, OSTEOBLASTS, INTERLEUKIN-7, BONE resorption, BONES

Abstract

The present study defines the function of nuclear factor of activated T cells (NFAT)c1 and NFATc2 in osteoblast function in vivo and in vitro. Nfatc1loxP/loxP, Nfatc2loxP/loxP, and Nfatc1loxP/loxP;Nfatc2loxP/loxP conditional mice were mated with BGLAP‐Cre transgenics to inactivate Nfatc1 and Nfatc2 singly and in combination in osteoblasts. Microcomputed tomography demonstrated that male and female conditionally inactivated Nfatc1, Nfatc2 and dual Nfatc1;Nfatc2 mice had osteopenia at Lumbar 3 (L3) sites when compared to littermate controls. However, the Nfatc1 and Nfatc2 inactivation singly and in combination in Bglap‐expressing osteoblasts did not result in an appreciable phenotype at femoral sites. Bone histomorphometry of L3 confirmed the osteopenic phenotype and demonstrated that Nfatc1;Nfatc2 inactivated male mice had a significant decrease in osteoblast number and in osteoblast surface and osteoid surface. The dual downregulation of Nfatc1 and Nfatc2 in bone marrow stromal cells caused a decrease in Alpl and Bglap expression, confirming a role of these transcription factors in osteoblast function. In conclusion, our studies reveal that NFATc1 and NFATc2 are necessary for optimal vertebral, but not femoral, bone homeostasis in vivo and osteoblast differentiation in vitro. [ABSTRACT FROM AUTHOR]

Published

2020

2. 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

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

Author

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

Published

2018

4. Glucocorticoids inhibit notch target gene expression in osteoblasts.

Author

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

Published

2018