Literature DB >> 35739380

Cav1.2 regulated odontogenic differentiation of NG2+ pericytes during pulp injury.

Yunyu Fu1,2, Yanqin Ju1, Shouliang Zhao3.   

Abstract

NG2+ pericytes, as the possible precursor cells of mesenchymal stem cells (MSCs), have drawn attention due to their ability to differentiate into odontoblasts. Cav1.2 is involved in the differentiation process of stem cells, but its role in the differentiation of NG2+ pericytes is not clear. The aim of the present study was to examine the role of Cav1.2 in the differentiation of NG2+ pericytes into odontoblasts. NG2+ pericytes were obtained from human dental pulp cells by magnetic-activated cell sorting. During the odontogenic differentiation of NG2+ pericytes, the effects of the Cav1.2 inhibitors, nimodipine and Cav1.2 knockdown shRNA, were analyzed by real-time polymerase chain reaction and alizarin red staining. NG2CreERT2/Rosa26-GFP lineage-tracing mice were established to further investigate the roles of NG2+ pericytes and Cav1.2 in incisor self-repair after injury in vivo. At 10 min, 1 day, and 3 days after pulp injuries in transgenic mice, NG2-GFP+ and Cav1.2 immunofluorescence co-staining was performed on the incisors. Nimodipine treatment and Cav1.2 knockdown showed similar inhibition of calcium nodule formation and mRNA levels of osteogenic markers (DSPP, DMP1, and Runx2, p < 0.05). NG2+ pericytes migrated from their inherent perivascular location to the odontoblast layers after pulp injury. Cav1.2 showed a similar response pattern as NG2+ pericytes and gradually returned to normal levels. In addition, many co-stained areas of Cav1.2 and NG2+ pericytes, both near the perivascular and odontoblast layers, were observed. These results indicate that Cav1.2 played a vital role in the odontogenic differentiation of NG2+ pericytes, and that it might be closely linked to the NG2+ pericytes-mediated repair of dental pulp injury in vivo.
© 2022. The Author(s), under exclusive licence to The Society of The Nippon Dental University.

Entities:  

Keywords:  Cav1.2; NG2+ pericytes; Nimodipine; Odontogenic differentiation; Pulp injuries

Year:  2022        PMID: 35739380     DOI: 10.1007/s10266-022-00720-w

Source DB:  PubMed          Journal:  Odontology        ISSN: 1618-1247            Impact factor:   2.634


  33 in total

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Journal:  Br Dent J       Date:  2013-10       Impact factor: 1.626

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Journal:  Cell Stem Cell       Date:  2018-07-05       Impact factor: 24.633

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Authors:  Songtao Shi; Stan Gronthos
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6.  Lipopolysaccharide upregulates the proliferation, migration, and odontoblastic differentiation of NG2+ cells from human dental pulp in vitro.

Authors:  Guofeng Yang; Yanqin Ju; Shangfeng Liu; Shouliang Zhao
Journal:  Cell Biol Int       Date:  2019-03-19       Impact factor: 3.612

7.  Perivascular Stem Cells at the Tip of Mouse Incisors Regulate Tissue Regeneration.

Authors:  Yvonne Wy Pang; Jifan Feng; Felipe Daltoe; Robert Fatscher; Eileen Gentleman; Molly M Gentleman; Paul T Sharpe
Journal:  J Bone Miner Res       Date:  2015-10-21       Impact factor: 6.741

8.  Composition of Mineral Produced by Dental Mesenchymal Stem Cells.

Authors:  A A Volponi; E Gentleman; R Fatscher; Y W Y Pang; M M Gentleman; P T Sharpe
Journal:  J Dent Res       Date:  2015-08-07       Impact factor: 6.116

9.  Glial origin of mesenchymal stem cells in a tooth model system.

Authors:  Nina Kaukua; Maryam Khatibi Shahidi; Chrysoula Konstantinidou; Vyacheslav Dyachuk; Marketa Kaucka; Alessandro Furlan; Zhengwen An; Longlong Wang; Isabell Hultman; Lars Ahrlund-Richter; Hans Blom; Hjalmar Brismar; Natalia Assaife Lopes; Vassilis Pachnis; Ueli Suter; Hans Clevers; Irma Thesleff; Paul Sharpe; Patrik Ernfors; Kaj Fried; Igor Adameyko
Journal:  Nature       Date:  2014-07-27       Impact factor: 49.962

10.  Pericyte-like progenitors show high immaturity and engraftment potential as compared with mesenchymal stem cells.

Authors:  Amina Bouacida; Philippe Rosset; Valérie Trichet; Fabien Guilloton; Nicolas Espagnolle; Thomas Cordonier; Dominique Heymann; Pierre Layrolle; Luc Sensébé; Frédéric Deschaseaux
Journal:  PLoS One       Date:  2012-11-07       Impact factor: 3.240

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