Periodontal Disease at the Biofilm-gingival Interface

Overview

Journal J Periodontol

Date 2007 Dec 7

PMID 18062113

Citations 77

Authors

S Offenbacher

S P Barros

R E Singer

K Moss

R C Williams

J D Beck

Affiliations

Soon will be listed here.

Abstract

Background: A molecular epidemiologic study provided the opportunity to characterize the biology of the biofilm-gingival interface (BGI) in 6,768 community-dwelling subjects.

Methods: 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%).

Results: 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.

Conclusions: 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.

Citing Articles

Meteorin-like levels of oral fluids in periodontal health and diseases: a comparative cross-sectional study.

Saglam E, Toraman A, Savran L, Saglam M, Koseoglu S Clin Oral Investig. 2025; 29(2):137.

PMID: 39964474 PMC: 11836087. DOI: 10.1007/s00784-025-06222-7.

Topical Biocomposites Based on Collagen, Hyaluronic Acid and Metronidazole as Periodontitis Treatment.

Albu Kaya M, Simonca A, Rau I, Coman A, Marin M, Popa L Pharmaceuticals (Basel). 2024; 17(10).

PMID: 39458977 PMC: 11510136. DOI: 10.3390/ph17101336.

Mobile Point-of-Care Device Using Molecularly Imprinted Polymer-Based Chemosensors Targeting Interleukin-1β Biomarker.

Park R, Jeon S, Lee J, Jeong J, Kwon Y, Kim S Biosensors (Basel). 2023; 13(12).

PMID: 38131773 PMC: 10741793. DOI: 10.3390/bios13121013.

Ageing and Inflammation: What Happens in Periodontium?.

Zhu L, Tang Z, Hu R, Gu M, Yang Y Bioengineering (Basel). 2023; 10(11).

PMID: 38002398 PMC: 10669535. DOI: 10.3390/bioengineering10111274.

Nuclear aberrations in the gingival epithelium of patients with chronic periodontitis.

Serikova O, Shumilovich B, Filippova Z, Kalaev V, Kalaeva E, Larina A J Indian Soc Periodontol. 2023; 27(4):374-380.

PMID: 37593557 PMC: 10431217. DOI: 10.4103/jisp.jisp_18_22.