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Title: Roles of L-type calcium channels (Ca_V1.2) and the distal C-terminus (DCT) in differentiation and mineralization of rat dental apical papilla stem cells (rSCAPs).
Author: Gao Q, Ge J, Ju Y, Li C, Gao J, Wu M, Zhao S.
Journal: Arch Oral Biol; 2017 Feb; 74():75-81. PubMed ID: 27918898.
Abstract:
OBJECTIVE: Voltage-gated inward Ca²⁺ currents (ICa) are triggered by cell depolarization and commonly produce transient increases in the cytoplasmic free Ca²⁺ concentration. The Ca_V1.2 distal C-terminus is susceptible to proteolytic cleavage, which yields a truncated Ca_V1.2 subunit and a cleaved C-terminal fragment (CCt or DCT). Stem cells from the apical papilla (SCAPs) has a capacity for differentiation into the odontoblastic-like cells in vitro and dentin forming in vivo, which makes SCAPs advantages in tissue engineering and regenerative endodontic. The aim of this study was to investigate the effect of Ca_V1.2 and its distal C-terminal fragment in the odontoblastic differentiation of rat SCAPs (stem cells from the apical papilla). DESIGN: In this study, we generated stable Ca_V1.2 knockdown and DCT over-expressed rSCAPs using short hairpin RNA and DCT gene containing Lentivirus vectors, respectively. The transfected apical papilla cells were induced to differentiate into the odontoblast-like cells, and the expression of markers for odontoblastic differentiation were analyzed by alizarin red staining, Real-time Polymerase chain reaction (RT-PCR), and Western blot analysis. RESULTS: The knockdown of Ca_V1.2 and excess expression of DCT both suppressed the expression of DSPP, ALP in mRNA level and the formation of calcium nodules. CONCLUSIONS: Our results suggest that Ca_V1.2 and DCT play important roles in the differentiation of rSCAPs, DCT might act as a transcription factor and regulate the differentiation of rSCAPs.

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