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Host Markers of Periodontal Diseases: Meta‐Analysis of Diagnostic Accuracy Studies

牙龈炎 医学 牙周炎 荟萃分析 生物标志物 内科学 曲线下面积 唾液 诊断生物标志物 诊断准确性 慢性牙周炎 二、侵袭性牙周炎 胃肠病学 牙科 生物 生物化学
作者
Mia Rakić,Elena Calciolari,Melissa M. Grant,Sandro Radovanović,Nagihan Bostancı,Philip M. Preshaw
出处
期刊:Journal of Clinical Periodontology [Wiley]
卷期号:52 (S29): 155-181 被引量:6
标识
DOI:10.1111/jcpe.14167
摘要

ABSTRACT Objective To identify host markers with optimal diagnostic performance for clinical implementation in the diagnosis of periodontal diseases and prediction of future disease progression and/or disease resolution. Material and Methods Cross‐sectional and prospective studies with ≥ 20 participants per group, reporting diagnostic accuracy (e.g., area under the curve [AUC]) of host markers for periodontal diagnosis (focused question 1 [FQ1]), periodontitis progression/relapse (FQ2) or resolution (FQ3) were searched in three electronic databases. Meta‐analyses estimating diagnostic accuracy (DA) for individual host markers and for grouped salivary and gingival crevicular fluid (GCF) markers independently were performed whenever two or more studies were identified. Results Sixty‐one eligible studies were identified, of which 13 were included in meta‐analyses for FQ1 (discrimination between health and periodontitis). Matrix metalloproteinase‐8 (MMP‐8) was the most reported biomarker in both saliva and GCF, with comparable AUC (0.70–0.90), sensitivity (0.49–0.84) and specificity (0.62–0.79) in both sample types. Cytokines had good ability for discrimination of periodontitis/gingivitis versus health, although they were substantially less accurate for periodontitis versus gingivitis. Combinations of cytokines and MMPs tended to increase overall diagnostic accuracy but without significant improvement in the case of periodontitis/gingivitis discrimination. Bone markers were the best performing group of salivary markers (AUC = 0.91) when compared to cytokines (AUC = 0.86) and MMPs (AUC = 0.77). GCF microRNAs (MiRs) were a singly meta‐analysed group of biomarkers demonstrating AUC = 0.79. Conclusion Reported studies on host periodontal markers exhibit serious limitations regarding clinical and validation standards, being the main cause for lack of progress in clinical implementation of biomarkers in periodontal classification. Disease‐specific markers such as bone markers showed better diagnostic performance (from limited number of studies) for the diagnosis of periodontitis when compared to cytokines and MMPs.
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