JAGGED1 stimulates cranial neural crest cell osteoblast commitment pathways and bone regeneration independent of canonical NOTCH signaling

Kamalakar, Archana; McKinney, Jay M.; Salinas Duron, Daniel; Amanso, Angelica M.; Ballestas, Samir A.; Drissi, Hicham; Willett, Nick J.; Bhattaram, Pallavi; García, Andrés J.; Wood, Levi B.; Goudy, Steven L.

Affiliations

¹Department of Otolaryngology, USA

²Wallace H. Coulter Department of Biomedical Engineering, USA

³George W. Woodruff School of Mechanical Engineering, Georgia Tech College of Engineering, Atlanta, GA, USA

⁴The Atlanta Veterans Affairs Medical Center Atlanta, GA, USA

⁵Department of Computer Science, Westminster College, Salt Lake City, UT, USA

⁶Department of Cell Biology, USA

⁷Department of Orthopaedics, Emory University, Atlanta, GA, USA

⁸Parker H. Petit Institute for Bioengineering and Biosciences, USA

⁹Department of Pediatric Otolaryngology, Children's Healthcare of Atlanta, Atlanta, GA, USA

Abstract and keywords

Craniofacial bone loss is a complex clinical problem with limited regenerative solutions. Currently, BMP2 is used as a bone-regenerative therapy in adults, but in pediatric cases of bone loss, it is not FDA-approved due to concerns of life-threatening inflammation and cancer. Development of a bone-regenerative therapy for children will transform our ability to reduce the morbidity associated with current autologous bone grafting techniques. We discovered that JAGGED1 (JAG1) induces cranial neural crest (CNC) cell osteoblast commitment during craniofacial intramembranous ossification, suggesting that exogenous JAG1 delivery is a potential craniofacial bone-regenerative approach. In this study, we found that JAG1 delivery using synthetic hydrogels containing O9–1 cells, a CNC cell line, into critical-sized calvarial defects in C57BL/6 mice provided robust bone-regeneration. Since JAG1 signals through canonical (Hes1/Hey1) and non-canonical (JAK2) NOTCH pathways in CNC cells, we used RNAseq to analyze transcriptional pathways activated in CNC cells treated with JAG1 ± DAPT, a NOTCH-canonical pathway inhibitor. JAG1 upregulated expression of multiple NOTCH canonical pathway genes (Hes1), which were downregulated in the presence of DAPT. JAG1 also induced bone chemokines (Cxcl1), regulators of cytoskeletal organization and cell migration (Rhou), signaling targets (STAT5), promoters of early osteoblast cell proliferation (Prl2c2, Smurf1 and Esrra), and, inhibitors of osteoclasts (Id1). In the presence of DAPT, expression levels of Hes1 and Cxcl1 were decreased, whereas, Prl2c2, Smurf1, Esrra, Rhou and Id1 remain elevated, suggesting that JAG1 induces osteoblast proliferation through these non-canonical genes. Pathway analysis of JAG1 + DAPT-treated CNC cells revealed significant upregulation of multiple non-canonical pathways, including the cell cycle, tubulin pathway, regulators of Runx2 initiation and phosphorylation of STAT5 pathway. In total, our data show that JAG1 upregulates multiple pathways involved in osteogenesis, independent of the NOTCH canonical pathway. Moreover, our findings suggest that JAG1 delivery using a synthetic hydrogel, is a bone-regenerative approach with powerful translational potential.

Keywords: JAGGED1; Intramembranous ossification; Bone regeneration; RNAseq; Non-canonical JAG1-NOTCH pathways

Links

DOI: 10.1016/j.bone.2020.115657

PubMed: 32980561

WoS: 000604734500015

History

Received: 2020-07-16

Revised: 2020-09-16

Accepted: 2020-09-16

Online: 2020-09-25

Cited Works (1)

Year	Entry
1995	Benjamini Y, Hochberg Y. Controlling the false discovery rate: a practical and powerful approach to multiple testing. J R Stat Soc B. 1995;57(1):289-300.