Literature DB >> 26494267

Cytotoxicity and osteogenic potential of silicate calcium cements as potential protective materials for pulpal revascularization.

Eduardo A Bortoluzzi1, Li-Na Niu2, Chithra D Palani3, Ahmed R El-Awady3, Barry D Hammond3, Dan-Dan Pei4, Fu-Cong Tian5, Christopher W Cutler3, David H Pashley3, Franklin R Tay6.   

Abstract

OBJECTIVES: In pulpal revascularization, a protective material is placed coronal to the blood clot to prevent recontamination and to facilitate osteogenic differentiation of mesenchymal stem cells to produce new dental tissues. Although mineral trioxide aggregate (MTA) has been the material of choice for clot protection, it is easily displaced into the clot during condensation. The present study evaluated the effects of recently introduced calcium silicate cements (Biodentine and TheraCal LC) on the viability and osteogenic differentiation of human dental pulp stem cells (hDPSCs) by comparing with MTA Angelus.
METHODS: Cell viability was assessed using XTT assay and flow cytometry. The osteogenic potential of hDPSCs exposed to calcium silicate cements was examined using qRT-PCR for osteogenic gene expressions, alkaline phosphatase enzyme activity, Alizarin red S staining and transmission electron microscopy of extracellular calcium deposits. Parametric statistical methods were employed for analyses of significant difference among groups, with α=0.05.
RESULTS: The cytotoxic effects of Biodentine and TheraCal LC on hDPSCs were time- and concentration-dependent. Osteogenic differentiation of hDPSCs was enhanced after exposure to Biodentine that was depleted of its cytotoxic components. This effect was less readily observed in hDPSCs exposed to TheraCal LC, although both cements supported extracellular mineralization better than the positive control (zinc oxide-eugenol-based cement). SIGNIFICANCE: A favorable tissue response is anticipated to occur with the use of Biodentine as a blood clot-protecting material for pulpal revascularization. Further investigations with the use of in vivo animal models are required to validate the potential adverse biological effects of TheraCal LC on hDPSCs.
Copyright © 2015 Academy of Dental Materials. Published by Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Biocompatibility; Calcium silicate cements; Cytotoxicity; Mineral trioxide aggregate; Revascularization

Mesh:

Substances:

Year:  2015        PMID: 26494267      PMCID: PMC4974822          DOI: 10.1016/j.dental.2015.09.020

Source DB:  PubMed          Journal:  Dent Mater        ISSN: 0109-5641            Impact factor:   5.304


  65 in total

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4.  On the history and mechanism of alizarin and alizarin red S stains for calcium.

Authors:  H Puchtler; S N Meloan; M S Terry
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6.  Fracture strength of bovine incisors after intra-radicular treatment with MTA in an experimental immature tooth model.

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10.  Effect of an Experimental Direct Pulp-capping Material on the Properties and Osteogenic Differentiation of Human Dental Pulp Stem Cells.

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