Abstract
Diabetes has been associated with periodontitis, but the mechanisms through which periodontal diseases affect the metabolic control remain unclear.
Objective:
This study aimed to evaluate serum leveis of inflammatory markers, IL-8, IL-6 and monocyte chemoattractant protein 1 (MCP-1), in type 2 diabetic patients in the presence of chronic periodontitis.
Material and Methods:
Forty two individuals were enrolled in this study and assigned to one of five groups: diabetes mellitus with inadequate glycemic control and periodontitis (DMI+P, n = 10), diabetes mellitus with adequate glycemic control and periodontitis (DMA+P, n = 10), diabetes mellitus without periodontitis (DM, n = 10), periodontitis without diabetes (P, n=6), and neither diabetes nor periodontitis (H, n = 6). Periodontal clinical examination included visible plaque index (PL), gingival bleeding index (GB), probing depth (PD), attachment level (AL) and bleeding on probing (BP). Glycemic control was evaluated by serum concentration of glycated hemoglobin (HbAlc). Inflammatory serum markers IL-8, IL-6 and (MCP-1) were measured by ELISA.
Results:
DMI+P and DMA+P groups presented higher PD (p=0.025) and AL (p=0.003) values when compared to the P group. There were no significant differences among groups for IL-6, IL-8 and MCP-1 serum levels.
Conclusions:
Although periodontitis was more severe in diabetic patients, the serum levels of the investigated inflammatory markers did not differ among the groups.
Diabetes mellitus; Periodontitis; Cytokines; Inflammation
INTRODUCTION
Type 2 diabetes mellitus (T2DM) is the most common endocrine disorder and its incidence is increasing worldwide. This condition is a serious public health concern due to the need for lifelong care, premature death and the fact that it remains incurable2222- Litwak L, Goh SY, Hussein Z, Malek R, Prusty V, Khamseh ME. Prevalence of diabetes complications in people with type 2 diabetes mellitus and its association with baseline characteristics in the multinational A1chieve study. Diabetol Metab Syndr. 2013;5(1):57.. It is characterized by a progressive deficient secretion and action of insulin. Insulin resistance, whereby target tissues do not respond to this hormone, is a characteristic of the disease's first phase, when there is often a corresponding hyperinsulinemia11- American Diabetes Association. Standards of medical care in diabetes - 2011. Diabetes Care. 2011;34(Suppl 1):S11-61.. This resistance comes together with inflammatory processes in the development of diabetes chronic complications3232- Sun WL, Chen LL, Zhang SZ, Wu YM, Ren YZ, Qin GM. Inflammatory cytokines, adiponectin, insulin resistance and metabolic control after periodontal intervention in patients with type 2 diabetes and chronic periodontitis. Intern Med. 2011;50(15):1569-74.. Among these complications, periodontal diseases (PD) are very common and immune modulating factors are necessary for pathogen clearance, but also contribute to host tissues damage, as those seen in PD.
Clues to the involvement of inflammation in diabetes date back to more than a century ago. Proinflammatory molecules as tumor necroses factor (TNF)-α, leptin, interleukin (IL)-6, resistin, monocyte chemoattractant protein-1 (MCP-1) and visfatin, among others, are expressed at high levels in activated macrophages and/or other cells. Proinflammatory cytokines such as TNF-α and IL-1β activate JNK and IKKβ/NF-κB through classical receptor-mediated mechanisms which are also activated by pattern recognition receptors, bound to substances as lipopolissacharide (LPS) from gram negative bacteria. These include the Toll Like Receptors (TLRs) and the receptor for advanced glycation end products (RAGE). Prolonged hyperglycemia and the accompanying production of excess amounts of advanced glycation end products (AGEs) can activate NF-κB. JNK promotes insulin resistance through the phosphorylation of serine residues in insulin receptor signaling (IRS)-1 that negatively regulates normal signaling through the insulin receptor/IRS-1 axis. NF-κB induces insulin resistance by promoting the expression of numerous target genes as those for TNF-α, IL-6, IL-8, MCP-1, MIP-1α, MIP-2, resistin, ICAM-1, VCAM-12929- Shoelson SE, Lee J, Goldfine AB. Inflammation and insulin resistance. J Clin Invest. 2006;116(7):1793-801..
The inflammation associated with PD, characterized by elevated pro-inflammatory cytokines, innate immune receptor expression, and cellular infiltrate is exacerbated in patients with T2DM where TLR-4 and RAGEs play a significant role and contribute to induce responses by oral epithelial cells22- Amir J, Waite M, Tobler J, Catalfamo DL, Koutouzis T, Katz J, et al. The role of hyperglycemia in mechanisms of exacerbated inflammatory responses within the oral cavity. Cell Immunol. 2011;272(1):45-52..
The local production of cytokines in response to periodontal bacteria and their products results in higher serum concentrations of pro-inflammatory biomarkers1313- Górska R, Gregorek H, Kowalski J, Laskus-Perendyk A, Syczewska M, Madalinski K. Relationship between clinical parameters and cytokine profiles in inflamed gingival tissue and serum samples from patients with chronic periodontitis. J Clin Periodontol. 2003;30(12):1046-52. and a poor glycemic control in T2DM patients is associated with a loss of mucosal barrier integrity and accumulation of innate immune receptor ligands resulting in an exacerbation of ongoing inflammation22- Amir J, Waite M, Tobler J, Catalfamo DL, Koutouzis T, Katz J, et al. The role of hyperglycemia in mechanisms of exacerbated inflammatory responses within the oral cavity. Cell Immunol. 2011;272(1):45-52..
Thus, the adverse effect of periodontitis in T2DM may be explained by an increase in systemic inflammation, which contributes to insulin resistance1919- Koromantzos PA, Makrilakis K, Dereka X, Offenbacher S, Katsilambros N, Vrotsos IA, et al. Effect of non-surgical periodontal therapy on C-reactive protein, oxidative stress, and matrix metalloproteinase (MMP)-9 and MMP-2 levels in patients with type 2 diabetes: a randomized controlled study. J Periodontol. 2012;83(1):3-10..
The interrelation between more severe PD and DM is established88- Costa FO, Miranda Cota LO, Pereira Lages EJ, Soares Dutra Oliveira AM, Dutra Oliveira PA, Cyrino RM, et al. Progression of periodontitis and tooth loss associated with glycemic control in individuals undergoing periodontal maintenance therapy: a 5-year follow-up study. J Periodontol. 2013;84(5):595-605.,3232- Sun WL, Chen LL, Zhang SZ, Wu YM, Ren YZ, Qin GM. Inflammatory cytokines, adiponectin, insulin resistance and metabolic control after periodontal intervention in patients with type 2 diabetes and chronic periodontitis. Intern Med. 2011;50(15):1569-74. and there are evidences on the importance of cytokine analysis in T2DM evolution2929- Shoelson SE, Lee J, Goldfine AB. Inflammation and insulin resistance. J Clin Invest. 2006;116(7):1793-801. and therapy blockade2121- Larsen CM, Faulenbach M, Vaag A, Ehses JA, Donath MY, Mandrup-Poulsen T. Sustained effects of interleukin-1 receptor antagonist treatment in type 2 diabetes. Diabetes Care. 2009;32(9):1663-8..
As chronic or recurring inflammation contributes to an aberrant continuation of acute phase response and may also lead to further diabetes complications, such as micro and macroangiopathy and impaired healing1414- Graves DT, Kayal RA. Diabetic complications and dysregulated innate immunity. Front Biosci. 2008;13(1):1227-39.,2828- Saremi A, Nelson RG, Reid M, Hanson RL, Sievers ML, Taylor GW, et al. Periodontal disease and mortality in type 2 diabetes. Diabetes Care. 2005;28(1):27-32., it is suggested that periodontal disease with increased inflammatory response at local and systemic levels3030- Southerland JH, Moss K, Taylor GW, Beck JD, Pankow J, Gangula PR, et al. Periodontitis and diabetes associations with measures of atherosclerosis and CHD. Atherosclerosis. 2012;222(1):196-201. may collaborate to insulin resistance present on T2DM pathogenesis. However, scientific evidence on the effects of chronic periodontitis on diabetes mellitus remains inadequate and inconclusive99- Chen L, Luo G, Xuan D, Wei B, Liu F, Li J, et al. Effects of non-surgical periodontal treatment on clinical response, serum inflammatory parameters, and metabolic control in patients with type 2 diabetes: a randomized study. J Periodontal. 2012;83(4):435-43.. Furthermore, whether periodontal therapy may help to control serum levels of inflammatory cytokines still remains controversial55- Behle JH, Sedaghatfar MH, Demmer RT, Wolf DL, Celenti R, Kebschull M, etal. Heterogeneity of systemic inflammatory responses to periodontal therapy. J Clin Periodontol. 2009;36(4):287-94.. While some studies showed an effective improvement in periodontal parameters, circulating inflammatory markers and glycemic control after periodontal treatment in patients with T2DM99- Chen L, Luo G, Xuan D, Wei B, Liu F, Li J, et al. Effects of non-surgical periodontal treatment on clinical response, serum inflammatory parameters, and metabolic control in patients with type 2 diabetes: a randomized study. J Periodontal. 2012;83(4):435-43.,1717- Kardegler L, Buduneli N, Cetinkalp S, Kinane DF. Adipokines and inflammatory mediators after initial periodontal treatment in patients with type 2 diabetes and chronic periodontitis. J Periodontol. 2010;81(1):24-33.,3232- Sun WL, Chen LL, Zhang SZ, Wu YM, Ren YZ, Qin GM. Inflammatory cytokines, adiponectin, insulin resistance and metabolic control after periodontal intervention in patients with type 2 diabetes and chronic periodontitis. Intern Med. 2011;50(15):1569-74., others have shown that these responses were inconsistent across individuals and not sustainable over time33- Auyeung L, Wang PW, Lin RT, Hsieh CJ, Lee PY, Zhuang RY, et al. Evaluation of periodontal status and effectiveness of non-surgical treatment in patients with type 2 diabetes mellitus in Taiwan for a 1-year period. J Periodontol. 2012;83(5):621-8.,55- Behle JH, Sedaghatfar MH, Demmer RT, Wolf DL, Celenti R, Kebschull M, etal. Heterogeneity of systemic inflammatory responses to periodontal therapy. J Clin Periodontol. 2009;36(4):287-94.,1919- Koromantzos PA, Makrilakis K, Dereka X, Offenbacher S, Katsilambros N, Vrotsos IA, et al. Effect of non-surgical periodontal therapy on C-reactive protein, oxidative stress, and matrix metalloproteinase (MMP)-9 and MMP-2 levels in patients with type 2 diabetes: a randomized controlled study. J Periodontol. 2012;83(1):3-10..
The elevated levels of systemic inflammatory mediators, such as IL-6, in obesity or metabolic syndrome enhance the host response to periodontal pathogens, hence increasing the chance of periodontal destruction. IL-6 is a multifunctional cytokine produced by a variety of cells including macrophages, neutrophils, and endothelial cells. The double edge effects (i.e., pro- and anti-inflammatory) of this molecule entail complexity in investigating its role and, until now, no evidence from animal or human studies supports the hypothetical model in which metabolic syndrome-induced IL-6 increases the risk of destructive periodontal disease1818- Khosravi R, Ka K, Huang T, Khalili S, Nguyen BH, Nicolau B, et al. Tumor necrosis factor- a and interleukin-6: potential interorgan inflammatory mediators contributing to destructive periodontal disease in obesity or metabolic syndrome. Mediators Inflamm. 2013;2013:728987..
Interleukin 8 (IL-8) is a chemokine important for recruiting neutrophils during healing and its levels were shown to be tightly linked to increased susceptibility to periodontitis1212- Figueredo CM, Gustafsson A. Increased amounts of laminin in GCF from untreated patients with periodontitis. J Clin Periodontol. 2000;27(5):313-8..
Monocyte chemoattractant protein 1 (MCP-1) is also thought to play an important role in inflammatory processes. It has been implicated as a key factor in recruitment and activation of peripheral blood leukocytes in atherosclerotic lesions and adipose tissue. Elevated levels of circulating MCP-1 have been found in patients with T2DM, and experimental data have shown that this protein increases macrophage infiltration, inflammation and insulin resistance in transgenic mice2626- Odegaard JI, Ricardo-Gonzalez RR, Goforth MH, Morel CR, Subramanian V, Mukundan L, et al. Macrophage-specific PPARgamma controls alternative activation and improves insulin resistance. Nature. 2007;447(7148):1116-20..
Some studies33- Auyeung L, Wang PW, Lin RT, Hsieh CJ, Lee PY, Zhuang RY, et al. Evaluation of periodontal status and effectiveness of non-surgical treatment in patients with type 2 diabetes mellitus in Taiwan for a 1-year period. J Periodontol. 2012;83(5):621-8.,66- Beisswenger PJ, Brown WV, Ceriello A, Le NA, Goldberg RB, Cooke JP, et al. Meal induced increases in C-reactive protein, interleukin-6 and tumour necrosis factor a are attenuated by prandial + basal insulin in patients with type 2 diabetes. Diabet Med. 2011;28(9):1088-95., 99- Chen L, Luo G, Xuan D, Wei B, Liu F, Li J, et al. Effects of non-surgical periodontal treatment on clinical response, serum inflammatory parameters, and metabolic control in patients with type 2 diabetes: a randomized study. J Periodontal. 2012;83(4):435-43.,1717- Kardegler L, Buduneli N, Cetinkalp S, Kinane DF. Adipokines and inflammatory mediators after initial periodontal treatment in patients with type 2 diabetes and chronic periodontitis. J Periodontol. 2010;81(1):24-33.,2424- Mealey B, Oates T; American Academy of Periodontology. Diabetes mellitus and periodontal diseases. J Periodontol. 2006;77(8):1289-303. have evaluated markers such as interleukin-6 (IL-6), tumor necrosis factor-a (TNF-α), C-reactive protein (CRP), and IL-1β and related them to insulin resistance2424- Mealey B, Oates T; American Academy of Periodontology. Diabetes mellitus and periodontal diseases. J Periodontol. 2006;77(8):1289-303. and glycemic control33- Auyeung L, Wang PW, Lin RT, Hsieh CJ, Lee PY, Zhuang RY, et al. Evaluation of periodontal status and effectiveness of non-surgical treatment in patients with type 2 diabetes mellitus in Taiwan for a 1-year period. J Periodontol. 2012;83(5):621-8.; however, their results are still conflicting.
Based on the evidences that IL-6, IL-8 and MCP-1 are important key markers of immune response, which have been considered as critical mediators of initiation, progression and/or suppression of chronic periodontitis, and that no previous study had analyzed this combination of mediators in groups with and without diabetes and periodontal disease, this study aimed to evaluate serum levels of inflammatory markers, IL-8, IL-6 and MCP-1, in type 2 diabetic patients in the presence of chronic periodontitis.
PATIENTS AND METHODS
This study was conducted between January 2012 and March 2013 in full accordance with the Helsinki Declaration of 1975, as revised in 2000. The study protocol and the informed consent form were reviewed and approved by the Biomedical Sciences Institute Ethics Committee (#011/CEP) from the University of São Paulo (São Paulo, Brazil). T2DM individuals were recruited from the Diabetes Center at the Federal University of São Paulo. Non-diabetic patients were recruited from the School of Dentistry, University of São Paulo. Detailed medical and dental history was obtained from all patients. All volunteers received full mouth periodontal clinical examination performed at six sites per tooth (excluding third molars) from a calibrated examiner (HPCA). Intraexaminer reliability for detecting PDs within 1 mm was >90%. The presence of supragingival biofilm was recorded as plaque index (PL), marginal gingival bleeding was recorded as gingival bleeding (GB); bleeding on probing (BP), probing depth (PD) and attachment level (AL) were also evaluated. The probe used was North Caroline (UNC-15, Hu-Friedy®, Chicago, IL, USA). PL, GB and BP were recorded as absent (0) or present (1). Inclusion criteria were: age ≥35 years, confirmed diagnosis of type 2 diabetes over 3 years (for individuals with T2DM), generalized moderate to severe chronic periodontitis (American Academy of Periodontology, 1998) (≥30% of sites with PD >4 mm and bleeding on probing) and ≥15 remaining teeth. Pregnant women, smokers, patients with Body Mass Index (BMI) >40 kg/m2 or who received periodontal therapy, antibiotic or antiseptic therapy 6 months prior to the study were excluded. Blood samples were obtained and glycated hemoglobin (HbA1c) levels were determined for all individuals at the clinical laboratory of the University of São Paulo Hospital. Approximately 5 ml of blood were collected by venipuncture in untreated tubes (BD Vacutainer Rapid Serum Tube, Becton Dickinson Co., São Paulo, SP, Brazil). Serum was obtained by centrifugation at 2,500 g for 2 minutes, aliquoted and stored at -80°C until further analysis. Quantitative measurement of IL-6, IL-8 and MCP-1 was assayed by enzyme-linked immunosorbent assay (Human Standard ELISA Development Kit, PeproTech Inc., Rocky Hill, CT, USA) and read out using a Micro Plate reader (Model 680, Bio-Rad Laboratories Inc., Hercules, CA, USA). Serum from each patient was tested in triplicate, and a calibration curve was added to each plate.
Forty-two individuals were enrolled in this study. Patients with T2DM and periodontitis were divided in two groups, as adequate glycemic control when HbA1c <8.0% (DMA+P, n = 10) and inadequate glycemic control when HbA1c ≥8.0% (DMI + P, n=10). The other 3 groups were composed of T2DM individuals without periodontitis (DM, n = 10), non-diabetic with periodontitis (P, n=6) and non-diabetic without periodontitis (H, n=6).
Periodontal clinical data were analyzed using appropriate statistical software (SPSS version 17.0 for Windows, SPSS Inc., Chicago, IL, USA) considering the individual as a study unit. The Kolmogorov-Smirnov test was used to test the variables normality distribution. Data were analyzed by non-parametric statistical methods since data were not normally distributed. Comparisons between groups were determined using Kruskal-Wallis test and Tukey test. Tests were based on median values with variability measures (25% and 75% quartiles). Results were considered statistically significant at p<0.05. For GB, PL and BOP data, percentages of positive sites were obtained per patient and, thereafter, median values were calculated for the groups. For PD and AL, measured by millimeters, percent frequency was first obtained per patient and, thereafter, as a median value for the group.
Data from ELISA were analyzed by Kruskal-Wallis and Dunn's Multiple Comparison Test (Prism 5.0 Project, Graph Pad Software Inc., La Jolla, CA, USA). Values were obtained per patient and a median value was calculated for each group.
RESULTS
A total of 546 patients were assessed for eligibility, and only 42 fulfilled the inclusion criteria (Figure 1).
Demographic and HbA1c data from each group are described in Table 1.
Demographic characteristics and glycated level (mean±standard deviation) for participants in each group
Table 2 provides periodontal clinical parameters for each group with periodontitis: DMI+P, DMA+P and P. There were significant differences between diabetic (DMI+P and DMA+P) and non-diabetic (P) for PD (p=0.04) and AL (p = 0.01) values indicating a more severe disease among the diabetic patients. The other clinicai parameters did not differ significantly among groups. Intergroup clinical parameters comparison for DMI + P and DMA+P showed no significant differences (data not shown).
There were no differences between groups for IL-6 (p=0.6351), IL-8 (p=0.9460) and MCP-1 (p=0.2987) sera leveis (Figure 2).
IL-6 (A), IL-8 (B) and MCP-1 (C) serum levels in patients without periodontitis and T2DM (H), patients with periodontitis and without T2DM (P), patients with T2DM and without periodontitis (DM), patients with T2DM with adequate glycemic control and periodontitis (DMA+P) and patients with T2DM with inadequate glycemic control and periodontitis (DMI+P). MCP-1=monocyte chemoattractant protein-1; IL-6=interleukin 6; IL-8=interleukin 8; T2DM=Type 2 diabetes mellitus.
DISCUSSION
The present study evaluated clinical and inflammatory parameters among groups with and without T2DM and/or periodontitis.
T2DM patients presented significantly higher PD and AL values when compared to group P, without diabetes and with periodontitis. This result is consistent with a number of cross-sectional and longitudinal studies1616- Heitz-Mayfield LJ. Disease progression: identification of high-risk groups and individuals for periodontitis. J Clin Periodontol. 2005;32(Suppl 6):196-209.,2020- Lalla E, Papapanou PN. Diabetes mellitus and periodontitis: a tale of two common interrelated diseases. Nat Rev Endocrinol. 2011;7(12):738-48.,3131- Southerland JH, Taylor GW, Moss K, Beck JD, Offenbacher S. Commonality in chronic inflammatory diseases: periodontitis, diabetes, and coronary artery disease. Periodontol 2000. 2006;40:130-43. which had shown that the increased severity of PD in T2DM patients is due to an interorgan crosstalk under inflammatory conditions1818- Khosravi R, Ka K, Huang T, Khalili S, Nguyen BH, Nicolau B, et al. Tumor necrosis factor- a and interleukin-6: potential interorgan inflammatory mediators contributing to destructive periodontal disease in obesity or metabolic syndrome. Mediators Inflamm. 2013;2013:728987..
The positive correlation between glycemic control and severity of periodontal disease has been reported in the literature88- Costa FO, Miranda Cota LO, Pereira Lages EJ, Soares Dutra Oliveira AM, Dutra Oliveira PA, Cyrino RM, et al. Progression of periodontitis and tooth loss associated with glycemic control in individuals undergoing periodontal maintenance therapy: a 5-year follow-up study. J Periodontol. 2013;84(5):595-605.,1515- Haseeb M, Khawaja KI, Ataullah K, Munir MB, Fatima A. Periodontal disease in type 2 diabetes mellitus. J Coll Physicians Surg Pak. 2012;22(8):514-8.,3434- Tanwir F, Tariq A. Effect of glycemic control on periodontal status. J Coll Physicians Surg Pak. 2012;22(6):371-4.. Thus, we had expected to find a significant relationship between HbA1c levels (representing adequate - HbA1c <8.0% - and inadequate - HbA1c ≥8.0% - glycemic control) and periodontitis severity (in terms of increased PD and BOP). However, the periodontal clinical parameters data did not differ according to the diabetes control, corresponding to DMA+P and DMI+P groups, respectively. We can speculate that, in order to observe correlation, we would need to consider a stricter glycemic control of individuals with T2DM, that is, HbA1c between 6.5 and 7.0%, which would hamper even more the group selection. Besides, HbA1c refers to glycemic control in the last 2 or 3 months and we do not know how the chronic glycemic control in these individuals was. We also have to point out that hyperglycemia is only one factor of the multifactorial process of periodontal disease.
There were no differences among IL-6 serum levels in the 5 groups analyzed. The role of
locally produced IL-6 in the periodontitis pathogenesis has been demonstrated44- Azuma MM, Samuel RO, Gomes-Filho JE, Dezan-Junior E, Cintra LT. The
role of IL-6 on apical periodontitis: a systematic review. Int Endod J. 2013. doi:
10.1111/iej.12196. Epub ahead of print.
https://doi.org/10.1111/iej.12196...
,2525- Nibali L, Fedele S, D'Aiuto F, Donos N. Interleukin-6 in oral
diseases: a review. Oral Dis. 2012;18(3):236-43., since high levels of this cytokine were detected in symptomatic large
lesions rather than in asymptomatic small lesions44- Azuma MM, Samuel RO, Gomes-Filho JE, Dezan-Junior E, Cintra LT. The
role of IL-6 on apical periodontitis: a systematic review. Int Endod J. 2013. doi:
10.1111/iej.12196. Epub ahead of print.
https://doi.org/10.1111/iej.12196...
. This cytokine is overexpressed in sites with PD mainly in patients without
diabetes and patients with well-controlled T2DM when compared with patients with poorly
controlled diabetes3535- Venza I, Visalli M, Cucinotta M, De Grazia G, Teti D, Venza M.
Proinflammatory gene expression at chronic periodontitis and peri-implantitis sites
in patients with or without type 2 diabetes. J Periodontol.
2010;81(1):99-108.. The effect of periodontal
treatment on IL-6 levels showed conflicting data, yielding a tendency toward a
decrease77- Correa FO, Gonçalves D, Figueredo CM, Bastos AS, Gustafsson A, Orrico
SR. Effect of periodontal treatment on metabolic control, systemic inflammation and
cytokines in patients with type 2 diabetes. J Clin Periodontol.
2010;37(1):53-8.,3232- Sun WL, Chen LL, Zhang SZ, Wu YM, Ren YZ, Qin GM. Inflammatory
cytokines, adiponectin, insulin resistance and metabolic control after periodontal
intervention in patients with type 2 diabetes and chronic periodontitis. Intern Med.
2011;50(15):1569-74. or increase in serum levels in T2DM patients3333- Talbert J, Elter J, Jared HL, Offenbacher S, Southerland J, Wilder
RS. The effect of periodontal therapy on TNF-alpha, IL-6 and metabolic control in
type 2 diabetics. J Dent Hyg. 2006;80(2):7-22.. Furthermore, a controversial study suggested an increase or no
change in serum IL-6 levels in obesity and metabolic syndrome1818- Khosravi R, Ka K, Huang T, Khalili S, Nguyen BH, Nicolau B, et al.
Tumor necrosis factor- a and interleukin-6: potential interorgan inflammatory
mediators contributing to destructive periodontal disease in obesity or metabolic
syndrome. Mediators Inflamm. 2013;2013:728987.. It should be noticed that T2DM individuals evaluated in the
present study were under treatment with insulin, which may have induced low levels of
inflammatory biomarkers such as IL-666- Beisswenger PJ, Brown WV, Ceriello A, Le NA, Goldberg RB, Cooke JP,
et al. Meal induced increases in C-reactive protein, interleukin-6 and tumour
necrosis factor a are attenuated by prandial + basal insulin in patients with type 2
diabetes. Diabet Med. 2011;28(9):1088-95.,2323- Mao XM, Liu H, Tao XJ, Yin GP, Li Q, Wang SK. Independent
antiinflammatory effect of insulin in newly diagnosed type 2 diabetes. Diabetes Metab
Res Rev. 2009;25(5):435-41., counteracting the
high levels induced by periodontal inflammation.
In the present study, there were no significant differences in the sera levels of the studied inflammatory markers, MCP-1 and IL-8, among the groups, although previous data demonstrated that both were overexpressed in the gingival tissue with chronic periodontitis3535- Venza I, Visalli M, Cucinotta M, De Grazia G, Teti D, Venza M. Proinflammatory gene expression at chronic periodontitis and peri-implantitis sites in patients with or without type 2 diabetes. J Periodontol. 2010;81(1):99-108.. A search in the literature revealed no study in humans regarding T2DM and/ or periodontitis and MCP-1 serum or gingival fluid levels. In rats experimental models, MCP-1 gingival crevicular fluid concentrations did not significantly differ between groups with diabetes and periodontitis and its levels were higher than in control healthy group2727- Sakallioglu EE, Ayas B, Lütfioglu M, Kele? GC, Açikgõz G, Firatli E. Gingival levels of monocyte chemoattractant protein-1 (MCP-1) in diabetes mellitus and periodontitis: an experimental study in rats. Clin Oral Investig. 2008;12(1):83-9..
High levels of IL-8 were shown in the gingival fluid of subjects with periodontal disease. However, subjects with T2DM presented significantly lower levels of IL-8 in the GCF when compared to healthy ones and there was no correlation between IL-8 gingival levels and HbA1c level1010- Duarte PM, Oliveira MC, Tambeli CH, Parada CA, Casati MZ, Nociti FH Jr. Overexpression of interleukin-1beta and interleukin-6 may play an important role in periodontal breakdown in type 2 diabetic patients. J Periodontal Res. 2007;42(4):377-81.,1111- Engebretson SP, Vossughi F, Hey-Hadavi J, Emingil G, Grbic JT. The influence of diabetes on gingival crevicular fluid beta-glucuronidase and interleukin-8. J Clin Periodontol. 2006;33(11):784-90.. Furthermore, IL-8 levels in serum tended to decrease after periodontal therapy in T2DM patients77- Correa FO, Gonçalves D, Figueredo CM, Bastos AS, Gustafsson A, Orrico SR. Effect of periodontal treatment on metabolic control, systemic inflammation and cytokines in patients with type 2 diabetes. J Clin Periodontol. 2010;37(1):53-8..
Due to the use of restrictive inclusion and exclusion criteria, in an attempt to minimize the occurrence of confounding factors, the small sample size is one limitation of this study. However, it is interesting to consider that some studies evaluated only specific dental sites through gingival crevicular fluid analysis, whereas the serum analysis provides a more valuable analysis of the inflammatory markers in the subject. To the best of our knowledge, there have been no studies evaluating these serum markers under all different conditions analyzed in this study.
Nevertheless, this study confirms the higher severity of periodontal disease in individuals with diabetes, highlighting the need for special oral healthcare for these patients. This study pointed out the great variability of the serum inflammatory biomarkers under all systemic and periodontal conditions studied. We can suggest that follow-up studies with stricter glycemic control and larger samples should be conducted in order to investigate the cumulative influence of periodontal conditions on serum inflammatory biomarkers in individuals with T2DM.
CONCLUSION
Although periodontitis was more severe in patients with diabetes, the serum levels of the investigated inflammatory markers were not different among the periodontitis patients.
Acknowledgement
We would like to thank Dr. Anna Carolina R. T. Horliana and Dr. Giovane H. Gomes for their collaboration in clinical procedures. This study was supported by São Paulo Research Foundation (FAPESP), São Paulo, Brazil, under protocol numbers 2011/18618-5; 10057-4; 06982-4.
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Publication Dates
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Publication in this collection
Mar-Apr 2014
History
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Received
28 Sept 2013 -
Reviewed
05 Dec 2013 -
Accepted
12 Dec 2013