Offenbacher S, Barros S P, Singer R E, Moss K, Williams R C, Beck J D
Center for Oral and Systemic Diseases and Department of Periodontology, School of Dentistry, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599-7455, USA.
J Periodontol. 2007 Oct;78(10):1911-25. doi: 10.1902/jop.2007.060465.
A molecular epidemiologic study provided the opportunity to characterize the biology of the biofilm-gingival interface (BGI) in 6,768 community-dwelling subjects.
Disease classifications and multivariable models were developed using clinical, microbial, inflammatory, and host-response data. The purpose was to identify new clinical categories that represented distinct biologic phenotypes based upon DNA checkerboard analyses of eight plaque bacteria, serum immunoglobulin G (IgG) titers to 17 bacteria, and the gingival crevicular fluid (GCF) levels of 16 inflammatory mediators. Five BGI clinical conditions were defined using probing depths (PDs) and bleeding on probing (BOP) scores. Subjects with all PDs < or = 3 mm were grouped as BGI-healthy (14.3% of sample) or BGI-gingivitis (BGI-G, 15.1%). Subjects with one or more PDs > or = 4 mm [deep lesion (DL)] were divided into low BOP (18.0%), moderate BOP (BGI-DL/MB, 39.7%), and severe BOP (BGI-DL/SB, 12.9%).
Subjects with BGI-G had increased levels of Campylobacter rectus-specific serum IgG levels (P = 0.01), and those with BGI-DL/SB had increased IgG levels to Porphyromonas gingivalis (P < 0.0003) and C. rectus (P < 0.01). BGI-DL/SB subjects had an excessive GCF interleukin (IL)-1beta and prostaglandin E2 response and an enhanced chronic inflammatory response with significant increases in GCF IL-6 and monocyte chemotactic peptide-1. Within BGI-DL/SB subjects, more severe pocketing and BOP were associated with higher levels of GCF IL-1beta, not higher microbial counts or plaque scores.
New BGI classifications create categories with distinct biologic phenotypes. The increased titers of C. rectus IgG among 68.5% of the BGI-G subjects and elevated P. gingivalis titers among BGI-DL/MB and BGI-DL/SB subjects (63.8% and 75.7%, respectively) are strongly supportive of the microbial specificity of pathogenesis for BGI categories.
一项分子流行病学研究为描述6768名社区居民生物膜-牙龈界面(BGI)的生物学特性提供了契机。
利用临床、微生物、炎症和宿主反应数据建立疾病分类和多变量模型。目的是基于对8种菌斑细菌的DNA棋盘分析、针对17种细菌的血清免疫球蛋白G(IgG)滴度以及16种炎症介质的龈沟液(GCF)水平,确定代表不同生物学表型的新临床类别。使用探诊深度(PD)和探诊出血(BOP)评分定义了5种BGI临床状况。所有PD≤3mm的受试者被归为BGI健康组(占样本的14.3%)或BGI牙龈炎组(BGI-G,占15.1%)。有一个或多个PD≥4mm[深度病变(DL)]的受试者被分为低BOP组(占18.0%)、中度BOP组(BGI-DL/MB,占39.7%)和重度BOP组(BGI-DL/SB,占12.9%)。
BGI-G受试者的直肠弯曲杆菌特异性血清IgG水平升高(P = 0.01),BGI-DL/SB受试者针对牙龈卟啉单胞菌(P < 0.0003)和直肠弯曲杆菌(P < 0.01)的IgG水平升高。BGI-DL/SB受试者的GCF白细胞介素(IL)-1β和前列腺素E2反应过度,慢性炎症反应增强,GCF IL-6和单核细胞趋化肽-1显著增加。在BGI-DL/SB受试者中,更严重的牙周袋深度和BOP与更高水平的GCF IL-1β相关,而不是更高的微生物计数或菌斑评分。
新的BGI分类创建了具有不同生物学表型的类别。68.5%的BGI-G受试者中直肠弯曲杆菌IgG滴度升高,BGI-DL/MB和BGI-DL/SB受试者中牙龈卟啉单胞菌滴度升高(分别为63.8%和75.7%),有力地支持了BGI类别发病机制的微生物特异性。
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