Cytotoxicity, Differentiation, and Biocompatibility of Root-End Filling: A Comprehensive Study

Author:

Jimenez-Bueno Ignacio1,Garcia-Contreras Rene2ORCID,Aranda-Herrera Benjamin2ORCID,Sakagami Hiroshi3ORCID,Lopez-Ayuso Christian Andrea2,Nakajima Hiroshi4,Jurado Carlos A.5ORCID,Nurrohman Hamid6ORCID

Affiliation:

1. Department of Endodontics, Faculty of Dentistry, Autonomous University State of Mexico (UAEMex), Toluca 50130, State of Mexico, Mexico

2. Interdisciplinary Research Laboratory, Nanostructures and Biomaterials Area, National School of Higher Studies (ENES) Leon, National Autonomous University of Mexico (UNAM), Leon 37684, Guanajuato, Mexico

3. Meikai University Research Institute of Odontology (M-RIO), Meikai University School of Dentistry, Sakado 350-0283, Saitama, Japan

4. Division of Dental Biomaterials Science, Department of Restorative and Biomaterials Sciences, Meikai University School of Dentistry, Sakado 350-0283, Saitama, Japan

5. Department of Prosthodontics, The University of Iowa College of Dentistry and Dental Clinics, Iowa City, IA 52242, USA

6. Department of Restorative Dentistry & Prosthodontics, University of Texas School of Dentistry, Houston, TX 77054, USA

Abstract

Assessing the biocompatibility of endodontic root-end filling materials through cell line responses is both essential and of utmost importance. This study aimed to the cytotoxicity of the type of cell death through apoptosis and autophagy, and odontoblast cell-like differentiation effects of MTA, zinc oxide–eugenol, and two experimental Portland cements modified with bismuth (Portland Bi) and barium (Portland Ba) on primary cell cultures. Material and methods: The cells corresponded to human periodontal ligament and gingival fibroblasts (HPLF, HGF), human pulp cells (HPC), and human squamous carcinoma cells from three different patients (HSC-2, -3, -4). The cements were inoculcated in different concentrations for cytotoxicity evaluation, DNA fragmentation in electrophoresis, apoptosis caspase activation, and autophagy antigen reaction, odontoblast-like cells were differentiated and tested for mineral deposition. The data were subject to a non-parametric test. Results: All cements caused a dose-dependent reduction in cell viability. Contact with zinc oxide–eugenol induced neither DNA fragmentation nor apoptotic caspase-3 activation and autophagy inhibitors (3-methyladenine, bafilomycin). Portland Bi accelerated significantly (p < 0.05) the differentiation of odontoblast-like cells. Within the limitation of this study, it was concluded that Portland cement with bismuth exhibits cytocompatibility and promotes odontoblast-like cell differentiation. This research contributes valuable insights into biocompatibility, suggesting its potential use in endodontic repair and biomimetic remineralization.

Funder

UNAM-DGAPA-PAPIME and PAPIIT

Publisher

MDPI AG

Subject

Molecular Medicine,Biomedical Engineering,Biochemistry,Biomaterials,Bioengineering,Biotechnology

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