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牙周病中 MnSOD 和过氧化氢酶表型与基因型的相关性。

Associations between the phenotype and genotype of MnSOD and catalase in periodontal disease.

机构信息

Division of Periodontics, Department of Dentistry, Taipei Medical University Hospital, Taipei Medical University, Taipei, 11031, Taiwan.

College of Public Health and Nutrition, Taipei Medical University, Taipei, 11031, Taiwan.

出版信息

BMC Oral Health. 2019 Aug 30;19(1):201. doi: 10.1186/s12903-019-0877-3.

Abstract

BACKGROUND

Periodontal disease is an inflammatory disease in which pathogenic infections trigger a series of inflammatory responses and redox regulation. The hypothesis of this study was that a host's redox regulation, as modified by genetic polymorphisms, may affect periodontal disease activities (including the plaque index (PlI), bleeding on probing (BOP), and pocket depth (PD)) during periodontal therapy.

METHODS

In total, 175 patients diagnosed with periodontitis were recruited from the Department of Periodontology, Taipei Medical University Hospital. Both saliva samples and clinical measurements (PlI, BOP, and PD) were taken at the baseline and at 1 month after completing treatment. Salivary manganese superoxide dismutase (MnSOD) and catalase, and corresponding genetic polymorphisms (MnSOD, T47C, rs4880 and Catalase, C-262 T, rs1001179) were determined. The extent of change (Δ) of MnSOD or catalase was calculated by subtracting the concentration after completing treatment from that at the baseline.

RESULTS

Subjects who carried the Catalase CC genotype had significantly higher salivary MnSOD or catalase levels. The MnSOD genotype had a significant effect on the percentage of PDs of 49 mm (p = 0.02), and salivary ΔMnSOD had a significant effect on the PlI (p = 0.03). The Catalase genotype had a significant effect on the PlI (p = 0.010.04), but the effect was not found for the mean PlI or PD. There was a significant interaction between the MnSOD genotype and salivary ΔMnSOD on PDs of 4~9 mm. After adjusting for gender, years of schooling, smoking status, and alcohol consumption, subjects with ΔMnSOD of < 0 μg/ml or Δcatalase of < 0 μg/ml had significantly higher 5.58- or 5.17-fold responses to scaling and root planing treatment.

CONCLUSIONS

The MnSOD T47C genotype interferes with the phenotype of salivary antioxidant level, alters MnSOD levels, and influences the PD recovery. MnSOD and catalase gene polymorphism associated with phenotype expression and susceptibility in periodontal root planing treatment responses.

摘要

背景

牙周病是一种炎症性疾病,其中致病感染会引发一系列炎症反应和氧化还原调节。本研究的假设是,宿主的氧化还原调节(由遗传多态性改变)可能会影响牙周病治疗期间的牙周病活动(包括菌斑指数(PlI)、探诊出血(BOP)和牙周袋深度(PD))。

方法

共招募了 175 名被诊断为牙周炎的患者,这些患者均来自台北医学大学附属医院牙周病科。在基线和治疗完成后 1 个月时,均采集了唾液样本和临床测量值(PlI、BOP 和 PD)。测定唾液锰过氧化物歧化酶(MnSOD)和过氧化氢酶及其相应的遗传多态性(MnSOD,T47C,rs4880 和 Catalase,C-262T,rs1001179)。通过从基线浓度中减去治疗后浓度来计算 MnSOD 或过氧化氢酶的变化程度(Δ)。

结果

携带过氧化氢酶 CC 基因型的受试者唾液 MnSOD 或过氧化氢酶水平显著升高。MnSOD 基因型对 4-9mm 的 PD 百分比有显著影响(p=0.02),唾液 ΔMnSOD 对 PlI 有显著影响(p=0.03)。Catalase 基因型对 PlI 有显著影响(p=0.01~0.04),但对平均 PlI 或 PD 无影响。MnSOD 基因型和唾液 ΔMnSOD 之间存在 PD 4-9mm 的显著交互作用。在校正性别、受教育年限、吸烟状况和饮酒状况后,ΔMnSOD<0μg/ml 或 Δ过氧化氢酶<0μg/ml 的患者对刮治和根面平整治疗的反应分别显著增加 5.58 倍和 5.17 倍。

结论

MnSOD T47C 基因型干扰唾液抗氧化水平的表型,改变 MnSOD 水平,并影响 PD 恢复。MnSOD 和过氧化氢酶基因多态性与牙周根面平整治疗反应中的表型表达和易感性相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bf99/6717336/da56e21497f5/12903_2019_877_Fig1_HTML.jpg

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