beta-Defensins are cationic antimicrobial peptides expressed in epithelia. They exhibit antibacterial, antifungal, and antiviral properties. Defensins are a component of the innate immune response, and it has been proposed that they have a protective role in the oral cavity. Previous studies have shown that human beta-defensin 1 (hBD-1) is constitutively expressed in oral epithelial cells but that expression varies between individuals. We tested the hypothesis that genetic variations in defensin peptide expression may be associated with opportunistic infections. This may be critical in the immunocompromised patient population, in which innate immune responses may have a relatively more important role. Oral Candida carriage status and the presence of six single-nucleotide polymorphisms (SNPs) in the DEFB1 gene encoding hBD-1 were evaluated in type I diabetic patients (n = 43) and nondiabetic controls (n = 50). Genomic DNA was obtained from buccal swabs. Portions of the DEFB1 gene were amplified, and each SNP was analyzed by a TaqMan assay, standardized with control DNA of known genotype. Candida carriage status was determined from unstimulated saliva on CHROMagar plating medium. A low level of Candida carriage was defined as < or = 350 CFU/ml. A high level of Candida carriage was seen in 44% of the diabetic subjects but only in 28% of the nondiabetic controls (P < 0.05). C. albicans predominated; however, diabetic subjects, especially those with high levels of carriage, showed an increased proportion of Candida glabrata and C. tropicalis. There was a strong association between an SNP in the 5' untranslated region (C-->G at position -44) and Candida carriage in both groups. Among individuals in the diabetic population who had the SNP allele 2 (G), 58% had low CFU, while 6% had high CFU. The C-->G SNP at position -44 is associated with low levels of Candida carriage. The resultant odd ratios are statistically significant for a protective effect (odd ratios, 25 for diabetic subjects and 8.5 for nondiabetic subjects). These results indicate that genetic variations in the DEFB1 gene encoding hBD-1 may have a major role in mediating and/or contributing to susceptibility to oral infection.

译文

β-防御素是在上皮细胞中表达的阳离子抗菌肽。它们具有抗菌,抗真菌和抗病毒特性。防御素是先天性免疫反应的组成部分,有人提出它们在口腔中具有保护作用。先前的研究表明,人β-防御素1(hBD-1)在口腔上皮细胞中组成性表达,但该表达因人而异。我们测试了防御素肽表达的遗传变异可能与机会性感染有关的假说。这在免疫受损的患者人群中可能是至关重要的,其中先天免疫应答可能具有相对更重要的作用。在I型糖尿病患者(n = 43)和非糖尿病对照(n = 50)中评估了口服念珠菌的运输状态以及在编码hBD-1的DEFB1基因中六个单核苷酸多态性(SNP)的存在。从颊拭子获得基因组DNA。扩增DEFB1基因的部分,并且通过TaqMan测定法分析每个SNP,所述TaqMan测定法用已知基因型的对照DNA标准化。从CHROMagar平板培养基上未刺激的唾液中确定念珠菌的运输状态。低水平的假丝酵母运输被定义为<或= 350 CFU / ml。在44%的糖尿病受试者中发现了高水平的念珠菌运输,但在28%的非糖尿病对照组中仅见(P <0.05)。白色念珠菌占主导地位;但是,糖尿病患者,尤其是携带量高的糖尿病患者,其光滑念珠菌和热带念珠菌的比例有所增加。两组中5'非翻译区的SNP(C-> G在-44位)和念珠菌运输之间有很强的联系。在具有SNP等位基因2(G)的糖尿病人群中,58%的CFU较低,而6%的CFU较高。 -44位的C-> G SNP与低水平的假丝酵母运输有关。所得的奇数比在保护作用方面具有统计学意义(奇数比,糖尿病患者为25,非糖尿病患者为8.5)。这些结果表明,编码hBD-1的DEFB1基因的遗传变异可能在介导和/或促进口腔感染的易感性中起主要作用。

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