4.5 Article

Analysis of the association of IL1B (C-511T) polymorphism with dental implant loss and the clusterization phenomenon

Journal

CLINICAL ORAL IMPLANTS RESEARCH
Volume 22, Issue 11, Pages 1235-1241

Publisher

WILEY
DOI: 10.1111/j.1600-0501.2010.02080.x

Keywords

dental implant loss; IL1 gene polymorphism; risk factors

Funding

  1. Instituto Latino Americano de Ensino e Pesquisa em Odontologia (ILAPEO), Curitiba, Brazil
  2. National Counsel of Technological and Scientific Development (CNPq) [475770/2004-8]

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Objectives: Endosteous dental implants consist in the treatment of choice to replace tooth loss. The knowledge that implant loss tends to cluster in subsets of individuals may indicate that host immune-inflammatory response is influenced by genetic factors. Interleukin-1 (IL-1) is a key mediator of inflammatory processes and functional polymorphisms in IL1 gene could be candidate genetic risk factors to study susceptibility to implant failure. The objective of this study was to investigate the association between IL1B (C-511T) genetic polymorphism and dental implant loss in a Brazilian population and its influence in the clusterization phenomenon. Material and methods: The sample composed of 277 unrelated, both gender, mean age 53.63 +/- 11.14 years individuals, divided into test group - 92 subjects with implant loss, and control group - 185 subjects with no implant loss. Patients' socioeconomic profile and clinical variables were investigated. Genomic DNA from oral mucosa was analyzed by polymerase chain reaction-restriction fragment length polymorphism. Results: There was significant difference between the groups in medical treatment (P = 0.040), edentulism (P = 0.019), and mean number of placed implants (P = 0.001). There was difference between groups with and without implant loss neither considering genotypes (P = 0.279) nor alleles (P = 0.168) for IL1B (C-511T) polymorphism. When individuals showing up to one implant failure (n = 254) were investigated vs. patients presenting multiple implant loss (n = 23), no difference was either observed between groups for genotype (P = 0.083) and allele (P = 0.838) frequencies. Conclusions: The borderline association of the study polymorphism with implant loss suggests further IL1 haplotype analysis to elucidate the global involvement of IL-1 proteins in the modulation of the osseointegration process.

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