Notch signaling regulates mineralization via microRNA modulation in dental pulp stem cells

Author:

Kulthanaamondhita Promphakkon1,Kornsuthisopon Chatvadee1,Chansaenroj Ajjima1,Suwittayarak Ravipha1,Trachoo Voraphat2,Manokawinchoke Jeeranan1,Lee Seung‐Cheol3ORCID,Egusa Hiroshi4,Kim Jin Man3,Osathanon Thanaphum1ORCID

Affiliation:

1. Center of Excellence for Dental Stem Cell Biology and Department of Anatomy, Faculty of Dentistry Chulalongkorn University Bangkok Thailand

2. Department of Oral and Maxillofacial Surgery, Faculty of Dentistry Chulalongkorn University Bangkok Thailand

3. Department of Oral Microbiology and Immunology School of Dentistry and Dental Research Institute Seoul National University Seoul Republic of Korea

4. Division of Molecular and Regenerative Prosthodontics Tohoku University Graduate School of Dentistry Sendai Miyagi Japan

Abstract

AbstractObjectivesThis study investigated the miRNA expression profile in Notch‐activated human dental stem pulp stem cells (DPSCs) and validated the functions of miRNAs in modulating the odonto/osteogenic properties of DPSCs.MethodsDPSCs were treated with indirect immobilized Jagged1. The miRNA expression profile was examined using NanoString analysis. Bioinformatic analysis was performed, and miRNA expression was validated. Odonto/osteogenic differentiation was examined using alkaline phosphatase staining, Alizarin Red S staining, as well as odonto/osteogenic‐related gene and protein expression.ResultsFourteen miRNAs were differentially expressed in Jagged1‐treated DPSCs. Pathway analysis revealed that altered miRNAs were associated with TGF‐β, Hippo, ErbB signalling pathways, FoxO and Ras signalling. Target prediction analysis demonstrated that 7604 genes were predicted to be targets for these altered miRNAs. Enrichment analysis revealed relationships to various DNA bindings. Among differentially expressed miRNA, miR‐296‐3p and miR‐450b‐5p were upregulated under Jagged1‐treated conditions. Overexpression of miR‐296‐3p and miR‐450b‐5p enhanced mineralization and upregulation of odonto/osteogenic‐related genes, whereas inhibition of these miRNAs revealed opposing results. The miR‐296‐3p and miR‐450b‐5p inhibitors attenuated the effects of Jagged1‐induced mineralization in DPSCs.ConclusionsJagged‐1 promotes mineralization in DPSCs that are partially regulated by miRNA. The novel understanding of these miRNAs could lead to innovative controlled mechanisms that can be applied to modulate biology‐targeted dental materials.

Publisher

Wiley

Subject

General Dentistry,Otorhinolaryngology

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