β-防御素 1（DEFB1）启动子区域的遗传变异与唇腭裂患儿高龋经验相关。

Genetic variation in the promoter region of beta-defensin 1 (DEFB 1) is associated with high caries experience in children born with cleft lip and palate.

机构信息

Department of Pediatric Dentistry, Riga Stradins University Institute of Stomatology , Riga, Latvia.

出版信息

Acta Odontol Scand. 2014 Apr;72(3):235-40. doi: 10.3109/00016357.2013.822549. Epub 2013 Aug 22.

DOI:10.3109/00016357.2013.822549

PMID:23964634

Abstract

OBJECTIVE

Caries is a common disease in humans and has a multifactorial etiology. It has been suggested that children born with cleft lip and/or palate (CL/P) have a higher susceptibility to caries, but data from several independent cohorts does not support this assumption. Previous work from our group suggested DEFB 1 is associated with higher caries experience. Since it is suspected that children born with CL/P have the same risk factors predisposing them to caries as other children of the same ages, the aim was to test if DEFB 1 was associated with caries experience in children born with CL/P.

MATERIALS AND METHODS

Sixty-nine children born with CL/P (aged 2-12 years) were included. Twenty-seven males and seven females had cleft lip and palate (CLP), six males and seven females had cleft lip (CL) and 13 males and nine females had cleft palate (CP). Caries was evaluated with the DMFT/dmft index by a calibrated evaluator. Two single nucleotide polymorphisms in DEFB 1 were selected (rs11362 and rs1800972) based on being associated with higher caries experience in previous work. Genotyping were carried out by real-time PCR using the Taqman assay method. The statistical analysis was performed between 'low-to-moderate caries experience group' and the 'high caries experience group'. Odds ratio calculations between caries experience and variant alleles and chi-square of Fisher exact tests at a level of significance of 0.05 were used.

RESULTS

There was no significant difference for caries experience between cleft types (p = 0.551). An association was found for the marker rs11362 and genotype distribution (p = 0.047). When analyzed in a recessive model, the genotype GG in this polymorphism increased the risk for caries susceptibility by more than 3-times (p = 0.031; OR = 3.16; 95% CI = 0.97-10.62).

CONCLUSION

The genetic variant rs11362 in DEFB 1 influences caries susceptibility in CL/P children. The results support the hypothesis that expression of DEFB 1 in saliva may serve as a biomarker for future caries risk.

摘要

目的

龋齿是一种常见的人类疾病，具有多因素病因。有人认为唇腭裂（CL/P）患儿更容易患龋齿，但来自几个独立队列的数据并不支持这一假设。我们之前的研究表明 DEFB1 与更高的龋齿经验有关。由于怀疑 CL/P 患儿与同龄儿童具有相同的龋齿易感性危险因素，因此本研究旨在测试 DEFB1 是否与 CL/P 患儿的龋齿经验有关。

材料和方法

纳入 69 例唇腭裂（CL/P）患儿（年龄 2-12 岁）。27 名男性和 7 名女性为唇腭裂（CLP），6 名男性和 7 名女性为唇裂（CL），13 名男性和 9 名女性为腭裂（CP）。由经过校准的评估员用 DMFT/dmft 指数评估龋齿。根据之前的研究结果，选择 DEFB1 中的两个单核苷酸多态性（rs11362 和 rs1800972）进行基因分型。采用 Taqman 检测方法进行实时 PCR 基因分型。采用 Fisher 精确检验进行统计分析，以 0.05 的显著性水平计算比值比（OR）。