生物陶瓷
牙本质
牙髓干细胞
材料科学
牙本质形成
活力测定
MTT法
骨钙素
牙本质涎磷蛋白
生物医学工程
脚手架
盖髓
牙科
干细胞
核化学
生物物理学
分子生物学
成牙本质细胞
化学
细胞生长
碱性磷酸酶
细胞生物学
纳米技术
细胞
生物化学
生物
医学
复合材料
酶
作者
Athina Bakopoulou,Eleni Papachristou,Maria Bousnaki,Christina Hadjichristou,Eleana Kontonasaki,Anna Theocharidou,Lambrini Papadopoulou,Nikolaos Kantiranis,George A. Zachariadis,Gabriele Leyhausen,Werner Geurtsen,Petros Koidis
标识
DOI:10.1016/j.dental.2016.05.013
摘要
This study aimed to investigate the potential of Mg-based bioceramic scaffolds combined with human treated-dentin matrices (hTDMs) and dentinogenesis-related morphogens to promote odontogenic differentiation and dentin-like tissue formation by Dental Pulp Stem Cells-DPSCs. DPSC cultures were established and characterized by flow cytometry. Experimental cavities were prepared inside crowns of extracted teeth and demineralized by EDTA (hTDMs). Zn-doped, Mg-based bioceramic scaffolds, synthesized by the sol–gel technique, were hosted inside the hTDMs. DPSCs were spotted inside the hTDMs/scaffold constructs with/without additional exposure to DMP-1 or BMP-2 (100 ng/ml, 24 h). Scanning Electron Microscopy-SEM, live/dead fluorescence staining and MTT assay were used to evaluate cell attachment and viability; Real time PCR for expression of osteo/odontogenic markers; Inductively Coupled Plasma-Atomic Emission Spectrometry-ICP/AES for scaffold elemental release analysis; ELISA for hTDM growth factor release analysis; SEM and X-ray Diffraction-XRD for structural/chemical characterization of the regenerated tissues. Scaffolds constantly released low concentrations of Mg2+, Ca2+, Zn2+ and Si4+, while hTDMs growth factors, like DMP-1, BMP-2 and TGFβ-1. hTDMs/scaffold constructs supported DPSC viability, inducing their rapid odontogenic shift, indicated by upregulation of DSPP, BMP-2, osteocalcin and osterix expression. Newly-formed Ca-P tissue overspread the scaffolds partially transforming into bioapatite. Exposure to DMP-1 or BMP-2 pronouncedly enhanced odontogenic differentiation phenomena. This is the first study to validate that combining the bioactivity and ion releasing properties of bioceramic materials with growth factor release by treated natural dentin further supported by exogenous addition of key dentinogenesis-related morphogens (DMP-1, BMP-2) can be a promising strategy for targeted dentin regeneration.
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