Sage Journals: Discover world-class research

Abstract

Periodontal diseases are common conditions in almost all age groups and a public health problem. Numerous risk factors have been demonstrated for this condition. The main mechanism of tissue destruction in the periodontitis is the functional interactions between microbial pathogens and host immune responses, thus cytokines have crucial roles in the pathogenesis periodontitis. Our previous study has demonstrated the susceptibility role of HLA-DRB1*04 allele in development of this disease. So, the individuals who were positive for HLA-DRB1*04 allele were excluded. We aimed to appraise the function of cytokines in the pathogenesis of periodontitis via assessment of tissue and blood levels of a number of cytokine coding genes, namely IL-1B, CXCL8, IL-17, IFNG, TGFB and TNFA1. Expressions of IFNG, IL-17, TGFB and TNFA1 were significantly higher in the peripheral blood of individuals with periodontitis compared with unaffected persons (Posterior beta $=$ 1.91, $P$ value $=$ 0.043; Posterior beta $=$ 1.84, $P$ value $=$ 0.033; Posterior beta $=$ 0.713, $P$ value $=$ 0.009 and Posterior beta $=$ 2.85, $P$ value $=$ 0.001, respectively). Moreover, expression of IL-17 was higher in females compared with males (Posterior beta $=$ 1.47, $P$ value $=$ 0.036). As the interaction effect between gender and group was remarkable for IL-17 expression, we further conducted subgroup analysis within gender group. Expression of IL-17 was higher in male patients compared with unaffected males (Posterior beta $=$ 1.9, $P$ value $=$ 0.048). We did not detect any significant difference in the expression of these cytokines in tissues obtained from affected individuals and unaffected controls. Therefore, our results imply dysregulation of cytokine coding genes in patients with periodontitis and warrant further mechanistical studies.

Keywords

Periodontitis cytokine IFNG IL-17 TGFB TNFA1

Get full access to this article

View all access options for this article.

References

Nazir

M.A.

, Prevalence of periodontal disease, its association with systemic diseases and prevention, Int J Health Sci (Qassim) 11 (2017), 72–80.

Cekici

Kantarci

Hasturk

and Van Dyke

T.E.

, Inflammatory and immune pathways in the pathogenesis of periodontal disease, Periodontol 2000 64 (2014), 57–80.

Hajishengallis

and Korostoff

J.M.

, Revisiting the Page & Schroeder model: The good, the bad and the unknowns in the periodontal host response 40 years later, Periodontol 2000 75 (2017), 116–151.

Darveau

R.P.

, Periodontitis: A polymicrobial disruption of host homeostasis, Nature Reviews. Microbiology 8 (2010), 481–490.

Hajishengallis

, Immunomicrobial pathogenesis of periodontitis: Keystones, pathobionts, and host response, Trends in Immunology 35 (2014), 3–11.

Graves

, Cytokines that promote periodontal tissue destruction, Journal of Periodontology 79 (2008), 1585–1591.

Pan

Wang

and Chen

, The cytokine network involved in the host immune response to periodontitis, International Journal of Oral Science 11 (2019), 1–13.

Figueredo

C.M.

Lira-Junior

and Love

R.M.

, T and B Cells in Periodontal Disease: New Functions in A Complex Scenario, Int J Mol Sci 20 (2019), 3949.

Wiebe

C.B.

and Putnins

E.E.

, The periodontal disease classification system of the American Academy of Periodontology-an update, Journal-Canadian Dental Association 66 (2000), 594–599.

10.

Lundmark

et al., Transcriptome analysis reveals mucin 4 to be highly associated with periodontitis and identifies pleckstrin as a link to systemic diseases, Scientific Reports 5 (2015), 1–13.

11.

Mazdeh

et al., Expression analysis of cytokine coding genes in epileptic patients, Cytokine 110 (2018), 284–287.

12.

Fiorillo

et al., Interferon crevicular fluid profile and correlation with periodontal disease and wound healing: A systemic review of recent data, Int J Mol Sci 19 (2018), 1908.

13.

Arjunkumar

et al., Comparative analysis of gingival crevicular fluid neopterin levels in health and periodontal disease: A biochemical study, Indian Journal of Dental Research: Official Publication of Indian Society for Dental Research 24 (2013), 582–586.

14.

Vernal

et al., Levels of interleukin-17 in gingival crevicular fluid and in supernatants of cellular cultures of gingival tissue from patients with chronic periodontitis, Journal of Clinical Periodontology 32 (2005), 383–389.

15.

Moutsopoulos

N.M.

et al., Porphyromonas gingivalis promotes Th17 inducing pathways in chronic periodontitis, Journal of Autoimmunity 39 (2012), 294–303.

16.

Fantini

M.C.

et al., Cutting edge: TGF-β induces a regulatory phenotype in CD4+ CD25- T cells through Foxp3 induction and down-regulation of Smad7, The Journal of Immunology 172 (2004), 5149–5153.

17.

Cardoso

C.R.

et al., Characterization of CD4+ CD25+ natural regulatory T cells in the inflammatory infiltrate of human chronic periodontitis, Journal of Leukocyte Biology 84 (2008), 311–318.

18.

Dutzan

Gamonal

Silva

Sanz

and Vernal

, Over-expression of forkhead box P3 and its association with receptor activator of nuclear factor-κ B ligand, interleukin (IL)-17, IL-10 and transforming growth factor-β during the progression of chronic periodontitis, Journal of Clinical Periodontology 36 (2009), 396–403.

19.

Kobayashi

et al., Induction of IL-10-producing CD4+ T-cells in chronic periodontitis, Journal of Dental Research 90 (2011), 653–658.

20.

McGeachy

M.J.

et al., TGF-β and IL-6 drive the production of IL-17 and IL-10 by T cells and restrain TH-17 cell-mediated pathology, Nature Immunology 8 (2007), 1390–1397.

21.

Ding

Chen

and Zhong

, TNF-α gene promoter polymorphisms contribute to periodontitis susceptibility: Evidence from 46 studies, Journal of Clinical Periodontology 41 (2014), 748–759.

22.

Madureira

D.F.

et al., Tumor necrosis factor-alpha in gingival crevicular fluid as a diagnostic marker for periodontal diseases: A systematic review, Journal of Evidence Based Dental Practice 18 (2018), 315–331.

23.

Górska

et al., Relationship between clinical parameters and cytokine profiles in inflamed gingival tissue and serum samples from patients with chronic periodontitis, Journal of Clinical Periodontology 30 (2003), 1046–1052.

24.

Fujihara

et al., Tumor necrosis factor-α enhances RANKL expression in gingival epithelial cells via protein kinase A signaling, Journal of Periodontal Research 49 (2014), 508–517.

25.

Kawai

et al., B and T lymphocytes are the primary sources of RANKL in the bone resorptive lesion of periodontal disease, The American Journal of Pathology 169 (2006), 987–998.

26.

Basso

F.G.

et al., Tumor Necrosis Factor-α and Interleukin (IL)-1β, IL-6, and IL-8 Impair In Vitro Migration and Induce Apoptosis of Gingival Fibroblasts and Epithelial Cells, Delaying Wound Healing, Journal of Periodontology 87 (2016), 990–996.

27.

Arancibia

et al., Tumor necrosis factor-α inhibits transforming growth factor-β-stimulated myofibroblastic differentiation and extracellular matrix production in human gingival fibroblasts, Journal of Periodontology 84 (2013), 683–693.

28.

Chen

R.-Y.

et al., Estradiol inhibits Th17 cell differentiation through inhibition of RORγT transcription by recruiting the ERα/REA complex to estrogen response elements of the RORγT promoter, J Immunol 194 (2015), 4019–4028.

29.

Khan

Dai

Karpuzoglu

and Ahmed

S.A.

, Estrogen increases, whereas IL-27 and IFN-gamma decrease, splenocyte IL-17 production in WT mice, Eur J Immunol 40 (2010), 2549–2556.

Transcript levels of cytokine coding genes in peripheral blood and tissues of patients with periodontitis

Abstract

Keywords

Get full access to this article

References