Your search keyword '"Jian H. Song"' showing total 3 results

1. Endothelial-to-osteoblast transition in normal mouse bone development

Author

Song-Chang Lin, Guoyu Yu, Yu-Chen Lee, Jian H. Song, Xingzhi Song, Jianhua Zhang, Theocharis Panaretakis, Christopher J. Logothetis, Yoshihiro Komatsu, Li-Yuan Yu-Lee, Guocan Wang, and Sue-Hwa Lin

Subjects

Biological sciences, Cell biology, Cancer, Science

Abstract

Summary: Metastatic prostate cancer (PCa) in bone induces bone-forming lesions. We have previously shown that PCa-induced bone originates from endothelial cells (ECs) that have undergone EC-to-osteoblast (OSB) transition. Here, we investigated whether EC-to-OSB transition also occurs during normal bone formation. We developed an EC and OSB dual-color reporter mouse (DRM) model that marks EC-OSB hybrid cells with red and green fluorescent proteins. We observed EC-to-OSB transition (RFP and GFP co-expression) in both endochondral and intramembranous bone formation during embryonic development and in adults. Co-expression was confirmed in cells isolated from DRM. Bone marrow– and lung-derived ECs underwent transition to OSBs and mineralization in osteogenic medium. RNA-sequencing revealed GATA family transcription factors were upregulated in EC-OSB hybrid cells and knockdown of GATA3 inhibited BMP4-induced mineralization. Our findings support that EC-to-OSB transition occurs during normal bone development and suggest a new paradigm regarding the endothelial origin of OSBs.

Published

2023

2. Multiple pathways coordinating reprogramming of endothelial cells into osteoblasts by BMP4

Author

Guoyu Yu, Pengfei Shen, Yu-Chen Lee, Jing Pan, Jian H. Song, Tianhong Pan, Song-Chang Lin, Xin Liang, Guocan Wang, Theocharis Panaretakis, Christopher J. Logothetis, Gary E. Gallick, Li-Yuan Yu-Lee, and Sue-Hwa Lin

Subjects

Molecular Biology, Cell Biology, Cancer, Science

Abstract

Summary: Cell type transition occurs during normal development and under pathological conditions. In prostate cancer bone metastasis, prostate cancer-secreted BMP4 induces endothelial cell-to-osteoblast (EC-to-OSB) transition. Such tumor-induced stromal reprogramming supports prostate cancer progression. We delineate signaling pathways mediating EC-to-OSB transition using EC lines 2H11 and SVR. We found that BMP4-activated pSmad1-Notch-Hey1 pathway inhibits EC migration and tube formation. BMP4-activated GSK3β-βcatenin-Slug pathway stimulates Osx expression. In addition, pSmad1-regulated Dlx2 converges with the Smad1 and β-catenin pathways to stimulate osteocalcin expression. By co-expressing Osx, Dlx2, Slug and Hey1, we were able to achieve EC-to-OSB transition, leading to bone matrix mineralization in the absence of BMP4. In human prostate cancer bone metastasis specimens and MDA-PCa-118b and C4-2b-BMP4 osteogenic xenografts, immunohistochemical analysis showed that β-catenin and pSmad1 are detected in activated osteoblasts rimming the tumor-induced bone. Our results elucidated the pathways and key molecules coordinating prostate cancer-induced stromal programming and provide potential targets for therapeutic intervention.

Published

2021

3. Multiple pathways coordinating reprogramming of endothelial cells into osteoblasts by BMP4

Author

Christopher J. Logothetis, Li Yuan Yu-Lee, Guoyu Yu, Jing Pan, Theocharis Panaretakis, Gary E. Gallick, Pengfei Shen, Guocan Wang, Song Chang Lin, Tianhong Pan, Xin Liang, Jian H. Song, Yu Chen Lee, and Sue Hwa Lin

Subjects

0301 basic medicine, animal structures, Stromal cell, Angiogenesis, Science, 02 engineering and technology, Article, 03 medical and health sciences, Prostate cancer, Prostate, medicine, Protein kinase B, Transcription factor, Molecular Biology, Cancer, Tube formation, Multidisciplinary, biology, Chemistry, Bone metastasis, Cell Biology, 021001 nanoscience & nanotechnology, medicine.disease, Cell biology, 030104 developmental biology, medicine.anatomical_structure, embryonic structures, Osteocalcin, biology.protein, Cancer research, 0210 nano-technology, Reprogramming

Abstract

Summary Cell type transition occurs during normal development and under pathological conditions. In prostate cancer bone metastasis, prostate cancer-secreted BMP4 induces endothelial cell-to-osteoblast (EC-to-OSB) transition. Such tumor-induced stromal reprogramming supports prostate cancer progression. We delineate signaling pathways mediating EC-to-OSB transition using EC lines 2H11 and SVR. We found that BMP4-activated pSmad1-Notch-Hey1 pathway inhibits EC migration and tube formation. BMP4-activated GSK3β-βcatenin-Slug pathway stimulates Osx expression. In addition, pSmad1-regulated Dlx2 converges with the Smad1 and β-catenin pathways to stimulate osteocalcin expression. By co-expressing Osx, Dlx2, Slug and Hey1, we were able to achieve EC-to-OSB transition, leading to bone matrix mineralization in the absence of BMP4. In human prostate cancer bone metastasis specimens and MDA-PCa-118b and C4-2b-BMP4 osteogenic xenografts, immunohistochemical analysis showed that β-catenin and pSmad1 are detected in activated osteoblasts rimming the tumor-induced bone. Our results elucidated the pathways and key molecules coordinating prostate cancer-induced stromal programming and provide potential targets for therapeutic intervention., Graphical abstract, Highlights • BMP4 upregulates several pathways essential for EC-to-OSB transition • BMP4 activates pSmad1-Notch-Hey1 and GSK3β-βcatenin-Slug-OSX pathways • pSmad1-regulated Dlx2 expression connects the pSmad1 and β-catenin pathways • Coexpression of OSX, Dlx2, Slug, and Hey1 is sufficient to induce EC-to-OSB transition, Molecular Biology ; Cell Biology ; Cancer

Published

2020