| Literature DB >> 23691333 |
Lina Bashour1, Razan Khattab, Elham Harfoush.
Abstract
Objective. To determine whether differences exist between periodontitis subjects with and without Coronary Heart Disease (CHD) in a Syrian population in the distribution of IL-1 alleles at positions IL-1α+4845, IL-1β+3954, IL-1β-511, and IL-1RN VNTR. Background. The role of Interleukin-1 genes in the association between periodontitis and CHD has been demonstrated in previous studies. No study has been carried out on the Syrian population to asses for such a role. Methods. 200 Syrian Arab periodontitis patients (184 males, 16 females; mean age 52.61) were divided into two groups: cases group 100 subjects with CHD (92 males, 8 females; mean age 52.06); controls group 100 subjects without CHD (92 males, 8 females; mean age 53.16). Probing depth (PD), clinical attachment loss (CAL), and alveolar bone loss (ABL) were performed for patients. Blood samples were collected for genotyping analysis of IL-1α+4845, IL-1β+3954, and IL-1β-511 using PCR-RFLP technique and IL-1RN VNTR using normal PCR. Results. An association between both (CAL and ABL) and CHD was shown after adjustment for other confounders (OR: 7.659, P = 0.001; OR: 3.645, P = 0.006, resp.). Also, an association between allele 2 of IL-1α+4845, IL-1β+3954, and IL-1β-511 and ABL was shown. Allele 2 of IL-1α+4845 and IL-1β-511 was associated with ABL among individuals with and without CHD. But after adjustment for other confounders, the association remained only between allele 2 of IL-11α+4845 and both CHD and severe ABL (OR: 0.189, P < 0.001). Conclusion. Allele 2 of IL-11α+4845 may be considered a risk indicator for having both CHD and severe ABL in the investigated Syrian population.Entities:
Year: 2013 PMID: 23691333 PMCID: PMC3649497 DOI: 10.1155/2013/195678
Source DB: PubMed Journal: ISRN Dent ISSN: 2090-4371
Genotyping of the four polymorphic variants.
| Gene/SNP | Primer sequences | Ta | RE | DT | DD | PCR product | HWE |
|---|---|---|---|---|---|---|---|
| IL-1 | FW: 5′-ATGGTTTTAGAAATCATCAAGCCTAGGGCA-3′ | 56 | SatI | 37 | 16 | 153 | 0.3124 |
| IL-1 | FW: 5′-CTCAGGTGTCCTCCAAGAAATCAAA-3′ | 57 | TaqI | 65 | 2 | 182 | 0.0591 |
| IL-1 | FW: 5′-TGGCATTGATCTGGTTCATC-3′ | 55 | AvaI | 37 | 16 | 304 | 0.547 |
| IL-1 RN VNTR | FW: 5′-CTCAGCAACACTCCTAT-3′ | 55 | 410 = 4 repeats | 0.562 |
SNP: single nucleotide polymorphisms; Ta: annealing temperature; HWE: the Hardy-Weinberg equilibrium; RE: restriction enzyme; DT: digestion temperature; DD: digestion duration; rs numbers are RefSNP SNP-identification codes as applied in the public nucleic acid polymorphism databases at the national center for biotechnology information [34].
Descriptive parameters and periodontal parameters in patients with and without CHD.
| Variable | CHD | Non-CHD | |
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| |
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| Age (years; mean ± SD) | 52.06 ± 6.899 | 53.16 ± 5.832 | 0.225† |
| Male (%) | 92% | 92% | 1.00† |
| Smokers (%) | 68% | 63% | 0.757† |
| BMI (Kg/m2; mean ± SD) | 26.17 ± 2.03 | 25.87 ± 1.91 | 0.005† |
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| PD (rank) | 106.11 | 94.90 | 0.158‡ |
| GR (rank) | 105.48 | 95.53 | 0.223‡ |
| CAL (rank) | 121.07 | 79.93 | <0.001‡ |
| ABL | |||
| Mild (%) | 8% | 12% | 0.016* |
| Moderate (%) | 40% | 56% | |
| Severe (%) | 52% | 32% | |
†Unpaired t-test.
‡Mann-Whitney U test
*X 2 test.
Genotype frequency of polymorphisms in the IL-1 gene cluster by CHD and Non-CHD.
| Genotype frequency | CHD | Non-CHD |
| ||
|---|---|---|---|---|---|
|
| % |
| % | ||
| IL-1 | |||||
| 1.1 | 64 | 64% | 37 | 37% | <0.001 |
| Combination 1.2 + 2.2 | 36 | 36% | 63 | 63% | |
| IL-1 | |||||
| 1.1 | 55 | 55% | 52 | 52% | 0.671 |
| Combination 1.2 + 2.2 | 45 | 45% | 48 | 48% | |
| IL-1 | |||||
| 1.1 | 43 | 43% | 40 | 40% | 0.667 |
| Combination 1.2 + 2.2 | 57 | 57% | 60 | 60% | |
| IL-1 RA VNTR | |||||
| 1.1 | 46 | 46% | 57 | 57% | 0.120 |
| Combination 1.2 + 2.2 | 54 | 54% | 43 | 43% | |
Genotype frequency of polymorphisms in the IL-1 gene cluster by the varying degrees of ABL.
| Alveolar bone loss | |||||||
|---|---|---|---|---|---|---|---|
| Genotype frequency | Mild | Moderate | Severe |
| |||
|
| % |
| % |
| % | ||
| IL-1 | |||||||
| 1.1 | 19 | 95% | 49 | 51% | 33 | 39% | <0.001 |
| Combination 1.2 + 2.2 | 1 | 5% | 47 | 49% | 51 | 61% | |
| IL-1 | |||||||
| 1.1 | 14 | 70% | 57 | 59% | 36 | 43% | 0.025 |
| Combination 1.2 + 2.2 | 6 | 30% | 39 | 41% | 48 | 57% | |
| IL-1 | |||||||
| 1.1 | 9 | 45% | 25 | 26% | 49 | 58% | <0.001 |
| Combination 1.2 + 2.2 | 11 | 55% | 71 | 74% | 35 | 42% | |
| IL-1 RA VNTR | |||||||
| 1.1 | 9 | 45% | 44 | 46% | 50 | 60% | 0.154 |
| Combination 1.2 + 2.2 | 11 | 55% | 52 | 54% | 34 | 40% | |
IL-1 genotypes of subjects with and without CHD by varying degrees of ABL.
| Alveolar bone loss | |||||||
|---|---|---|---|---|---|---|---|
| Genotype frequency | Mild | Moderate | Severe |
| |||
|
| % |
| % |
| % | ||
| IL-1 | |||||||
| CHD | |||||||
| 1.1 | 7 | 88% | 31 | 78% | 26 | 50% | 0.009 |
| Combination 1.2 + 2.2 | 1 | 12% | 9 | 22% | 26 | 50% | |
| Non-CHD | |||||||
| 1.1 | 12 | 100% | 18 | 32% | 7 | 22% | <0.001 |
| Combination 1.2 + 2.2 | 0 | 0% | 38 | 68% | 25 | 78% | |
| IL-1 | |||||||
| CHD | |||||||
| 1.1 | 5 | 63% | 27 | 68% | 23 | 44% | 0.070 |
| Combination 1.2 + 2.2 | 3 | 37% | 13 | 32% | 29 | 56% | |
| Non-CHD | |||||||
| 1.1 | 9 | 75% | 30 | 54% | 13 | 41% | 0.133 |
| Combination 1.2 + 2.2 | 3 | 25% | 26 | 46% | 19 | 59% | |
| IL-1 | |||||||
| CHD | |||||||
| 1.1 | 5 | 63% | 9 | 23% | 29 | 56% | 0.003 |
| Combination 1.2 + 2.2 | 3 | 37% | 31 | 77% | 23 | 44% | |
| Non-CHD | |||||||
| 1.1 | 8 | 33% | 32 | 29% | 40 | 63% | <0.001 |
| Combination 1.2 + 2.2 | 16 | 67% | 80 | 71% | 24 | 37% | |
| IL-1 RA VNTR | |||||||
| CHD | |||||||
| 1.1 | 5 | 63% | 14 | 35% | 27 | 52% | 0.107 |
| Combination 1.2 + 2.2 | 3 | 37% | 26 | 65% | 25 | 48% | |
| Non-CHD | |||||||
| 1.1 | 4 | 33% | 30 | 54% | 23 | 72% | 0.054 |
| Combination 1.2 + 2.2 | 8 | 67% | 26 | 46% | 9 | 28% | |
Multiple logistic regression with backward stepwise elimination.
| Significant variable |
|
|---|---|
| BMI | 0.002 |
| ABL (moderate + severe) | 0.001 |
| Allele 2 of IL-1 | <0.001 |
Outcome variable is CHD.
Full model was allele 2 of IL-1α +4845, allele 2 of IL-1β +3954, allele 2 of IL-1β −511, allele 2 of IL-1 RN VNTR, age, gender, smoking, BMI, PD, GR, CAL, and ABL.
Multiple logistic regression with backward stepwise elimination.
| Significant variable |
|
|---|---|
| Age | 0.015 |
| BMI | <0.001 |
| CAL | 0.006 |
| Allele 2 of IL-1a+4845 | <0.001 |
Outcome variable is CHD and (moderate + severe) ABL.
Full model was allele 2 of IL-1α +4845, allele 2 of IL-1β +3954, allele 2 of IL-1β −511, allele 2 of IL-1 RN VNTR, age, gender, smoking, BMI, PD, GR, and CAL.