Effect of Compounds of Galla Chinensis on Remineralisation of Initial Enamel Carious Lesions in Vitro

Overview

Journal J Dent

Publisher Elsevier

Specialty Dentistry

Date 2007 Jan 2

PMID 17196320

Citations 18

Authors

J P Chu

J Y Li

Y Q Hao

X D Zhou

Affiliations

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Abstract

Objective: To evaluate the effect of compounds of Galla chinensis on the remineralisation of initial enamel carious lesions in vitro.

Methods: Sixty bovine enamel blocks with early lesions were prepared and randomly divided into six treatment groups. The lesions were subjected to a pH-cycling regime for 12 days. Each daily cycle included 4x1min applications with one of six treatments; 1000ppm F aq. (as NaF, positive control); deionized water (negative control); or 4000ppm aqueous solutions of four G. chinensis extracts (GCEs); GCE, GCE-B, GCE-B1, or GCE-B2. Surface enamel microhardness was measured on the enamel blocks before and after demineralisation, and after pH-cycling, and percentage surface microhardness recovery (%SMHR) was calculated. The enamel specimens were then sectioned (thickness ca. 80microm) and examined by polarized light microscopy.

Results: All samples rehardened significantly compared to baseline. Fluoride had a significantly greater effect than all other treatments. In the GCEs groups, %SMHR was significantly greater than DDW for the GCE, GCE-B and GCE-B1 groups. There was no significant difference between the GCE-B2 group and DDW. Polarized light microscopy showed that the thickness of the surface layer increased obviously in all specimens including NaF group, GCE group, GCE-B group and GCE-B1 group. Negative birefringent band appeared in the lesions body and the depth of the lesions was obviously reduced.

Conclusion: The present study has demonstrated the potential of three GCEs (GCE, GCE-B and GCE-B1) to effect net rehardening of artificial carious lesions under dynamic pH-cyclic conditions.

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In vitro study of the treatment of dentin hypersensitivity with gallic acid combined with sodium fluoride.

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Barbosa C, Monici Silva I, Dame-Teixeira N J Appl Oral Sci. 2024; 32:e20240013.

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