Association between the +104T/C polymorphism in the 5'UTR of GDF5 and susceptibility to knee osteoarthritis: A meta-analysis
- Authors:
- Published online on: November 12, 2012 https://doi.org/10.3892/mmr.2012.1179
- Pages: 485-488
Abstract
Introduction
Knee osteoarthritis, the most common type of osteoarthritis, is a chronic degeneration of the articular cartilage around a joint. This disease commonly affects individuals over 45 years of age but has been identified in all age groups. In a previous study, the prevalence of knee osteoarthritis was identified as 12.2% and was significantly higher in females (14.9%) than in males (8.7%). Prevalence was revealed to increase with age (1). A variety of risk factors have been correlated with knee osteoarthritis: age, obesity, female gender, trauma, repetitive knee trauma, muscle weakness, joint laxity, mechanical forces, kneeling, squatting and miniscal injuries (2,3). In addition, various genetic polymorphisms may be associated with knee osteoarthritis (4).
Previous studies have demonstrated that growth differentiation factor 5 (GDF 5), a member of the transforming growth factor-β (TGF-β) superfamily, is important in musculoskeletal processes, affecting endochondral ossification, synovial joint and bone formation (5,6). The +104T/C polymorphism (rs143383) in the 5′ untranslated region (UTR) of GDF5 affects transcriptional activity in the GDF5 gene core promoter and transcriptional activity was found to be reduced in subjects carrying the T allele (6). An association between the +104T/C polymorphism and knee osteoarthritis was previously demonstrated (7–12). However, published results have been inconsistent. In this study, we performed a meta-analysis to investigate whether or not the +104T/C polymorphism is associated with knee osteoarthritis risk.
Materials and methods
Selection of studies
Data were independently gathered in duplicate by two investigators on the basis of a standard protocol. Discrepancies were settled by discussion until a consensus was reached. A literature search was conducted for studies that examined associations between the +104T/C polymorphism and knee osteoarthritis. A search was performed on PubMed, Google Scholar and the China National Knowledge Infrastructure database using the following keywords: ‘5′-UTR or GDF5’, ‘+104T/C polymorphism or genotype’ and ‘knee osteoarthritis’.
Selection criteria
To be eligible for inclusion in this meta-analysis, the following criteria were established: i) case-control study that addressed knee osteoarthritis cases and healthy controls; ii) studies that evaluated the association between +104T/C polymorphism and knee osteoarthritis risk; iii) studies that included sufficient genotype data for extraction; and iv) the genotype distribution among the control population in Hardy-Weinberg equilibrium (HWE).
Data extraction
The following information was extracted from the eligible studies: i) first author; ii) year of publication; iii) country; iv) ethnicity; v) sample size of subjects with and without CAD; vi) genotype distribution of subjects with and without knee osteoarthritis; and vii) P-value for HWE test in subjects without knee osteoarthritis.
Statistical analysis
Crude odds ratios (ORs) with 95% confidence intervals (CIs) were calculated to estimate the strength of correlation between the +104T/C polymorphism and knee osteoarthritis risk. The pooled ORs were performed under a homozygote comparison (TT vs. CC), a heterozygote comparison (TT vs. TC), a dominant model (CC+TC vs. TT) and a recessive model (TT+TC vs. CC). In addition, we conducted a stratification analysis in Asian and European individuals to explore and explain diversity among the results of various studies (7). We tested whether genotype frequencies of controls were in HWE using the Chi-square test. Q- and I2 tests were performed to evaluate whether the variation was due to heterogeneity or chance. If heterogeneity was identified among the studies (I2<50%), the pooled OR was estimated by the fixed-effects model. Otherwise, the random-effects model was used to estimate the pooled OR. Sensitivity analysis was performed through the random-effects model values compared with the fixed-effects to ensure the stability of the results. Publication bias was assessed by Begg's test (P<0.05 was considered to indicate a statistically significant difference). Analyses were performed using STATA version 12.0 (Stata Corporation, College Station, TX, USA). All P-values were two-sided.
Results
Characteristics of studies
A total of 33 studies were obtained by the literature search, among which 6 fit the inclusion criteria (8–13). The flowchart of reviews demonstrates the detailed process of selection (Fig. 1). Of the 25 excluded studies, 21 were not associated with +104T/C polymorphism, 1 did not have sufficient genotype data for extraction, 1 was a meta-analysis and 2 were reviews. Data were collected from 2,744 knee osteoarthritis patients and 4,518 controls. Genotype distributions among the controls of all included studies were consistent with HWE. The 6 included studies contained 8 population studies of 5 Asian and 3 Caucasian groups. Information from these studies and the number of cases and controls with TT, TC and CC genotypes reported in each are shown in Table I.
Results of meta-analysis
A summary of the meta-analysis findings of the association between +104T/C polymorphism and knee osteoarthritis risk is shown in Table II. Overall, we found a significant association of +104T/C polymorphism with knee osteoarthritis risk (TT vs. CC: OR 1.68, 95% CI=1.41–2.01; TT vs. TC: OR 1.18, 95% CI=1.01–1.38; dominant model: OR 0.72, 95% CI=0.61–0.86). In the subgroup analysis based on ethnicity, studies were divided into Caucasian and Asian populations. The same association was observed in the Caucasian (TT vs. CC: OR 1.45, 95% CI=1.13–1.85) and Asian (TT vs. CC: OR 1.99, 95% CI=1.53–2.60; TT vs. TC: OR 1.33, 95% CI=1.16–1.52; dominant model: OR 0.64, 95% CI=0.56–0.72; recessive model: OR 1.77, 95% CI=1.37–2.29) groups. Sensitivity analysis was performed through random-effects model values compared with the fixed-effects, the results of which indicated no statistically significant difference, rendering the values of meta-analysis valid (TT vs. CC: OR 1.68, 95% CI=1.40–2.01; TT vs. TC: OR 1.19, 95% CI=1.07–1.32; dominant model: OR 0.74, 95% CI=0.67–0.81; recessive model: OR 0.28, 95% CI=0.25–0.32). Publication bias of the studies was assessed using the funnel plot and Begg's test. Publication bias was not observed in the funnel plot (all P>0.05, Table II and Fig 2).
Discussion
The association of genetic polymorphism and knee osteoarthritis has recently attracted growing attention. Miyamoto et al were the first study group to investigate the association between +104T/C polymorphism in the 5′-UTR of GDF5 and knee osteoarthritis in Asians. The results showed a significant correlation between +104T/C polymorphism and knee osteoarthritis risk in Japanese and Chinese populations. More recent studies have confirmed this correlation between +104T/C polymorphism and susceptibility to knee osteoarthritis. However, a number of studies have also demonstrated a conflicting correlation. In the present study, we quantitatively assessed the correlation between +104T/C polymorphism and knee osteoarthritis risk. Six studies were included with a total of 2,744 knee osteoarthritis patients and 4,518 controls. Overall, a significant correlation was observed between the +104T/C polymorphism and knee osteoarthritis risk in Caucasian (TT vs. CC: OR 1.45, 95% CI=1.13–1.85) and Asian (TT vs. CC: OR 1.99, 95% CI=1.53–2.60; TT vs. TC: OR 1.33, 95% CI=1.16–1.52; dominant model: OR 0.64, 95% CI=0.56–0.72; recessive model: OR 1.77, 95% CI=1.37–2.29) individuals. No evidence was found for publication bias in this meta-analysis for the +104T/C polymorphism. As the eligible study number was limited in the meta-analysis, these results require further investigation.
The mechanistic correlation between the +104T/C polymorphism and knee osteoarthritis risk remains unclear. GDF5 is involved in articular cartilage development, regeneration and maintenance and is a specific marker for synovial joints of appendicular skeletons (14). The +104T/C polymorphism regulates transcriptional activity in the GDF5 gene core promoter and the T allele reveals reduced transcriptional activity, this SNP may be the biological basis for the alteration in function (8). This evidence suggests that the +104T/C polymorphism is important in the development of knee osteoarthritis.
Several potential limitations of the present study should be noted. First, the results may be affected by additional confounding factors, including gender and age. We were unable to perform gender- and age-related subgroup analyses due to incomplete data. Second, the effect of genetic and environmental interactions was not addressed in our meta-analysis. Third, the number of studies and subjects in the studies included in the meta-analysis by specific subgroups was small. Therefore, additional studies with larger sample sizes are required.
In conclusion, the present study indicates that +104T/C polymorphism in the 5′-UTR of GDF5 is associated with risk of knee osteoarthritis. However, further studies of gene-gene and gene-environment interactions should be taken into consideration to investigate this correlation.
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