- Research
- Open access
- Published:
Association between APOA5 polymorphisms and susceptibility to metabolic syndrome: a systematic review and meta-analysis
BMC Genomics volume 25, Article number: 590 (2024)
Abstract
Background
The association between Apolipoprotein A5 (APOA5) genetic polymorphisms and susceptibility to metabolic syndrome (MetS) has been established by many studies, but there have been conflicting results from the literature. We performed a meta-analysis of observational studies to evaluate the association between APOA5 gene polymorphisms and the prevalence of MetS.
Methods
PubMed, Web of Science, Embase, and Scopus were searched up to April 2024. The random effects model was used to estimate the odds ratios (ORs) and 95% confidence intervals (CI) of the association between APOA5 gene polymorphisms and the prevalence of MetS development. The potential sources of heterogeneity were evaluated by subgroup analyses and sensitivity analyses.
Results
A total of 30 studies with 54,986 subjects (25,341 MetS cases and 29,645 healthy controls) were included. The presence of rs662799 and rs651821 polymorphisms is associated with an approximately 1.5-fold higher likelihood of MetS prevalence (OR = 1.42, 95% CI: 1.32, 1.53, p < 0.001; I2 = 67.1%; P-heterogeneity < 0.001; and OR = 1.50, 95% CI: 1.36–1.65, p < 0.001), respectively. MetS is also more prevalent in individuals with the genetic variants rs3135506 and rs2075291. There was no evidence of a connection with rs126317.
Conclusion
The present findings suggest that polymorphisms located in the promoter and coding regions of the APOA5 gene are associated with an increased prevalence of MetS in the adult population. Identifying individuals with these genetic variations could lead to early disease detection and the implementation of preventive strategies to reduce the risk of MetS and its related health issues. However, because the sample size was small and there was evidence of significant heterogeneity for some APOA5 gene polymorphisms, these results need to be confirmed by more large-scale and well-designed studies.
Background
Metabolic syndrome (MetS) is a group of risk factors for cardiovascular disease, which include dyslipidemia, hypertension, hyperglycemia, and obesity, particularly central adiposity [1]. According to existing estimates, MetS is prevalent in approximately 31% of the world’s population [2]. MetS is associated with a 4-fold increase in coronary artery disease events [3] and a 1.2-fold increase in overall mortality [4]. Additionally, the prevalence of some cancers [5,6,7,8] higher in people with MetS compared to the general population. Given the high prevalence of MetS and its health effects, it is critical to understand the factors that influence its development.
In addition to the influence of environmental factors such as diet and exercise, inherited genetic variation is also a significant component in MetS development [9]. Single nucleotide polymorphisms (SNPs), the most common type of genetic variation, are likely to increase the risk of MetS.
The position of SNPs can determine how they affect the structure and quantity of gene products, which could explain the difference in susceptibility to various diseases [10]. Some SNPs located in a coding area or promoter region could explain the difference in susceptibility to various diseases [11]. Genome-wide association studies (GWAS) have identified several candidate genes, including apolipoprotein A5 (APOA5), which may influence susceptibility to metabolic syndrome (MetS) and its components [12,13,14].
The APOA5 locus is on chromosome 11q23 and has 4 exons that code for APOA5. It is next to the APOA1/APOC3/APOA4 gene cluster. APOA5, a 366 amino acid protein identified in triglyceride (TG)-rich lipoproteins and high density lipoprotein (HDL) particles [15,16,17,18], is a potent regulator of plasma TG and HDL-C levels [19].
Several SNPs in APOA5 have been reported to have significant effects on MetS components. The most commonly reported polymorphisms to be associated with TG levels, plasma HDL levels, and other MetS traits are − 1131T > C, c56C > G, and c553G > T [19,20,21,22].
So far, three meta-analyses have been published on the relationship between APOA5 polymorphisms and MetS [23,24,25]. In the past decade, there were two meta-analysis published [23, 24], but then 16 new studies related to the topic were published [15, 19, 21, 22, 25,26,27,28,29,30,31,32,33,34,35,36]. The other meta-analysis [25] has only focused on the North African population. Furthermore, in these meta-analyses, only two common polymorphisms, including − 1131T > C and c56C > G, have been examined [23,24,25]. While recent studies evaluated the association of emerging polymorphisms, such as c553G > T, -3 A > G, -12238T > C, and c1259T > C with MetS [19, 21, 22, 26, 35]. Hence, the results of these studies are not conclusive and should be interpreted with caution. Considering the limitations of previous meta-analyses and the importance of scientific updates in this field, the present study was conducted to investigate the relationship between different APOA5 variants and MetS in the adult population through a systematic review and meta-analysis of observational studies.
Methods
Our systematic review and meta-analysis were performed according to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) [37]. We have registered the protocol of this systematic review on the PROSPERO website (registration number: CRD42023461249).
Search strategy
The electronic databases PubMed, Web of Science, Embase, and Scopus were searched before April 15, 2024, to find studies that looked into the link between APOA5 gene polymorphisms and MetS risk in adults. Also, we have not considered any restrictions on the language or publication date. The references from the selected eligible articles and previous meta-analyses were screened for other relevant articles. The complete strategy, from searching in the databases to selecting eligible studies, is shown in Supplementary Table S1.
Inclusion and exclusion criteria
Studies were included if they met all of the following criteria: (1) all published observational studies (cross-sectional, cohort, case-control, and baseline of controlled clinical trials) that were done on adults; (2) showed a link between at least one APOA5 polymorphism and the prevalence of metabolic syndrome; (3) gave either the odds ratio (OR) and 95% confidence intervals (CI) or enough information to calculate OR and CI; and (4) used a validated definition to make the MetS diagnosis.
If studies were conducted on the same population, the study with a larger sample size was selected. Studies were excluded if they were performed among pregnant or lactating women, or if they lacked sufficient data to determine allele or genotype frequencies for APOA5. Two authors (SM and SMEM) screened the title, abstract, and full text of all retrieved references based on inclusion and exclusion criteria.
Data extraction
The following data were extracted by two authors (SM, SMEM) and then cross-checked by a second author (SS): the first author, year of publication, country, age, gender, number of total participants and number of participants with MetS, the definition of MetS, genotyping method, the presence of HWE and APOA5 variants, and confounding factors.
Risk of bias assessment
The quality of each study was assessed using the Newcastle-Ottawa (NOS) scale with a maximum score of 9 [38]. According to the scale, studies were classified into three levels: high quality (7–9 points), medium (4–6 points), and low quality (1–3 points).
Statistical analysis
The ORs and their 95% CIs of the prevalence of metabolic syndrome among polymorphisms of the apolipoprotein APOA5 gene were extracted from each study. The natural logarithm scale of OR and its CI as the effect size were included in the meta-analysis under two possible genetic models: the dominant model and the recessive model. For studies that did not provide sufficient data for meta-analysis, we calculated the ORs and 95% CIs as the odds of having metabolic syndrome in the variant allele-positive genotypes versus wild-type homozygous genotype (aa + Aa vs. AA) in the dominant model and metabolic syndrome in the variant homozygous genotype vs. the rest (aa vs. AA + Aa) in the recessive model with approaches that suggested in previous studies [39, 40]. The effect size was pooled by the DerSimonian and Laird method [41] using the random effects model, which assumes within-study sampling errors and between-study variances. Statistical heterogeneity between studies was evaluated using Cochran’s Q test and I-squared (I2) [42]. The heterogeneity was regarded as low, moderate, and high when the I2 values were 25%, 50%, and exceeded 75%, respectively [43]. To explore the potential sources of heterogeneity, subgroup analyses were conducted, stratified by geographic location, sex, study quality, sample size, MetS definition, and adjustment for potential confounding factors (including age, BMI, and smoking). Subgroup analysis was performed only for the dominant models. The deviation from HWE for each study was assessed for the control group using the chi-squared test. The sensitivity analyses were conducted by excluding studies from the meta-analysis one by one to test the robustness of each association. Possible publication bias was assessed using Egger’s test [44] and Begg’s test [45], with the results considered to indicate publication bias at P < 0.10. We also visually checked funnel plots for asymmetry. All statistical analyses were performed using STATA, version 17 (Stata Corp., College Station, TX). P values less than 0.05 were considered statistically significant.
Results
Literature search
Our initial search yielded 730 articles, of which 242 were duplicates and 416 were unrelated after screening the title or abstract. After evaluating 71 full-text articles, 39 were excluded (reasons provided in Supplementary Table S2). The update search identified one additional eligible article, resulting in a final selection of 30 studies for the meta-analysis [11, 15, 19, 21, 22, 24,25,26,27,28,29,30,31,32,33,34,35,36, 46,47,48,49,50,51,52,53,54,55,56,57].
Six studies were also included for systematic review because the number of studies related to other APOA5 polymorphisms was insufficient for meta-analyses [19, 50, 58,59,60]. The study screening process is shown in Fig. 1.
Flow diagram for the eligible study selection process
Studies characteristics
The general characteristics of the included studies are shown in Table 1. Our meta-analysis contained a total of 54,986 subjects, including 25,341 MetS cases and 29,645 healthy controls. All studies have cross-sectional design. Most studies were from Asia (n = 17) [11, 15, 22, 24, 26, 29,30,31,32, 34,35,36, 48, 49, 52, 55, 57] and Europe (n = 8) [27, 33, 46, 47, 50, 51, 54, 56], while we found just one study that was conducted in the USA [53], and four studies that were from Africa [19, 21, 25, 28]. The age range of the participants was 18 to 79, and the majority of studies were performed among both sexes, while three studies included only women [31, 32, 51]. Twenty-two studies were consistent with Hardy-Weinberg equilibrium (HWE) [11, 21, 22, 24, 25, 27, 29, 30, 32,33,34,35, 46, 48,49,50,51, 53,54,55,56,57]. However, in three studies, HWE was not in equilibrium [15, 36, 47], and in six studies, HWE was not reported [19, 24, 26, 28, 31, 52]. Seventeen studies used NCEP ATP III criteria [11, 22, 27, 28, 31,32,33,34, 46, 47, 49,50,51,52,53,54, 56], ten studies used IDF criteria [15, 19, 21, 24, 25, 29, 30, 35, 36, 48], and three studies used modified definition for identifying MetS [26, 55, 57]. Several techniques were used to identify the genotypes, such as the Polymerase Chain Reaction -Amplification Refractory Mutation System (PCR-RFLP) [15, 19, 22, 28, 31, 46, 48,49,50, 54, 56], Real-Time PCR Taqman [27, 33, 34, 51, 53], PCR and sequence-specific oligonucleotide probes (PCR-SSOP) [11, 30, 57], Mass Array [29, 52, 55], Matrix-Assisted Laser Desorption/Ionization (MALDI-TOF) [35, 47], Kaspar technology [21, 25], SNP Integration Tool (SNP-IT) assay [32], and bead-based microarray tech [24, 26, 36].
Quality assessment
The findings of the quality evaluation revealed that 23 of the included studies were of high quality [15, 19, 21, 22, 24,25,26,27, 29, 30, 33,34,35,36, 46, 47, 49,50,51,52,53, 55, 57], while five were of moderate level [11, 28, 32, 48, 54]. The remaining studies were found to have low quality [31, 56] (Supplementary Table S3).
Association between rs662799 (-1131 T > C) and MetS
The meta-analysis of the association between rs662799 polymorphism and MetS (n = 24 studies, 19,019 MetS and 22,438 controls) revealed a significant relationship between rs662799 polymorphism and the MetS prevalence in the dominant model (OR = 1.42, 95% CI: 1.32, 1.53; I2 = 68.7%; P-heterogeneity < 0.001) (Fig. 2) and recessive models (OR = 1.80, 95% CI: 1.65, 1.96; I2 = 0%; P-heterogeneity = 0.65). (Table 2) [11, 15, 19, 22, 24, 25, 27,28,29,30,31,32,33,34,35,36, 47, 49,50,51, 53,54,55,56]. There is a slightly more pronounced increase in studies conducted in females and studies that used IDF criteria for MetS definition. Subgroup analysis indicated that the relationship was found in Africa (OR = 3.92, 95% CI: 1.35, 11.39, P-heterogeneity = 0.002), Asia (OR = 1.56, 95% CI: 1.54, 1.57, P-heterogeneity = 0.74), and East Asia (OR = 1.44, 95% CI: 1.36, 1.53, P-heterogeneity = 0.22). The findings of subgroup analyses are shown in Supplementary Table S4.
Prevalence of metabolic syndrome associated with rs662799. The black square and horizontal line represent the study-specific odds ratio (OR) and 95% CI, respectively; the area of the black square is proportional to the specific-study weight to the overall meta-analysis. The center of the open diamond presents the pooled OR and its width represents the pooled 95% CI. Weights are from random-effects analysis
Association between rs3135506 (c56 C > G) and MetS
The pooled results of the 8 studies (3876 MetS and 5633 controls) showed that rs3135506 is significantly related to increased MetS prevalence in the dominant model (OR = 1.37, 95% CI: 1.21, 1.55; I2 = 0%, P-heterogeneity = 0.74) (Fig. 3) and association was not significant in the recessive model (OR = 1.93, 95% CI: 0.97, 3.85; I2 = 0%; P-heterogeneity = 0.88) (Table 2) [19, 21, 46, 47, 50, 51, 53, 54]. The results of subgroup analyses are shown in Supplementary Table S5.
Prevalence of metabolic syndrome associated with rs3135506. The black square and horizontal line represent the study-specific odds ratio (OR) and 95% CI, respectively; the area of the black square is proportional to the specific-study weight to the overall meta-analysis. The center of the open diamond presents the pooled OR and its width represents the pooled 95% CI. Weights are from random-effects analysis
Association between rs651821 (− 3 A > G), rs2075291 (c 553 G > T), rs126317 (-12,238 T > C) and MetS
The APOA5 polymorphism rs651821 was shown to be positively associated with MetS prevalence in both dominant (OR = 1.50, 95% CI: 1.36, 1.65; I2 = 25.5%, P-heterogeneity = 0.25) (Fig. 4 (A)) and recessive models (OR = 1.82, 95% CI: 1.56, 2.13; I2 = 0%, P-heterogeneity = 0.71) (Table 2) [21, 26, 35, 52, 57]. Additionally, the rs2075291 polymorphism was found to be associated with MetS risk in the dominant model (OR = 1.43, 95% CI: 1.14, 1.81; I2 = 40.8%, P-heterogeneity = 0.18) (Fig. 4(B)) [19, 35, 57]. However, no significant relationship between MetS risk and polymorphisms rs126317 (dominant model OR = 1.08, 95% CI: 0.79, 1.47, I2 = 86.9, %, P-heterogeneity < 0.001) (Fig. 4(C)), and recessive model OR = 0.97, 95% CI: 0.70, 1.34, I2 = 84.3, P-heterogeneity < 0.001) were observed (Table 2) [22, 46, 48]. Due to the low number of original studies included in the present meta-analysis for this polymorphism, we could not perform subgroup analysis to explore the sources of heterogeneity.
Prevalence of metabolic syndrome associated with rs651821 (A), rs2075291 (B), rs126317 (C). The black square and horizontal line represent the study-specific odds ratio (OR) and 95% CI, respectively; the area of the black square is proportional to the specific-study weight to the overall meta-analysis. The center of the open diamond presents the pooled OR and its width represents the pooled 95% CI. Weights are from random-effects analysis
Publication bias and sensitivity analyses
The pooled ORs were not altered by omitting any single study in the dominant model for rs662799 and rs3135506, indicating that our results were statistically robust. In addition, further analysis revealed that heterogeneity for rs662799 under dominant model remained constant even after excluding studies with a sample size of less than 100 (OR = 1.41, 95% CI: 1.31, 1.51, I² = 68.6%, P-heterogeneity < 0.001) [19, 28], a high sample size (OR = 1.41, 95% CI: 1.30, 1.53, I² = 69.9%, P-heterogeneity < 0.001) [36], obese people (OR = 1.43, 95% CI: 1.32, 1.55, I² = 68.3%, P-heterogeneity < 0.001) [27, 36], and and those conducted exclusively in postmenopausal women (OR = 1.40, 95% CI: 1.30, 1.51, I² = 70.4%, P-heterogeneity < 0.001) [31, 32].
No publication bias was observed in the association rs662799 with MetS (Egger’s test, P = 0.12 and Begg’s test, P = 0.21) and rs3135506 with MetS (Egger’s test, P = 0.14 and Begg’s test, P = 0.12) in dominant model.
Association between other APOA5 SNPs and MetS
After reviewing the included studies, it was discovered that there are other APOA5 variants that may be involved in the MetS susceptibility. Two studies showed a strong positive association between rs2266788 and the risk of MetS [59, 60]. While Ajjemami and colleagues did not report any significant association between this variant and MetS [19]. Since the mentioned studies did not provide enough data, it was not possible to perform a meta-analysis for this SNP. Flores-Viveros et al. [58], and Kisfali et al. [50], investigations have identified rs964184 and IVS3 + G476A as genetic variants that are associated with an increased risk of MetS. However, no significant association was found between rs17120035, rs9804646, rs1729410, or rs633389 and the development of MetS [55].
Discussion
Principle findings
The current meta-analysis revealed substantial associations between certain APOA5 polymorphisms, including rs662799 and rs651821, in both dominant and recessive models, as well as the dominant models of rs3135506 and rs2075291. Studies that investigated the dominant model of rs662799 polymorphism showed a slightly more pronounced increase in MetS prevalence among females, as did studies that used IDF criteria for MetS definition. However, the recessive models of rs3135506 and rs2075291, as well as both the dominant and recessive models of rs126317, did not show any association with MetS.
Comparison with previous meta-analyses
The polymorphisms rs662799 and rs3135506 have been investigated in previous meta-analyses regarding the risk of MetS [23,24,25]. In these meta-analyses, the mentioned SNPs have been shown to be associated with an increased risk of MetS, consistent with our findings. However, as mentioned previously, these meta-analyses had some limitations [23,24,25]. Firstly, these meta-analyses were published in the past decade [23, 24], and but 16 studies were published after that [15, 19, 21, 22, 25,26,27,28,29,30,31,32,33,34,35,36]. Secondly, some of these meta-analyses were specifically focused on a certain demographic, namely the African population [25]. Consequently, the generalizability of their findings is restricted. The present work is the first meta-analysis to evaluate the relationship between other APOA5 SNPs, such as rs651821, rs2075291, and rs126317, and the risk of MetS.
Potential underlying mechanisms
The results of our study show that polymorphisms located in the promoter area (rs662799 and rs651821) and the codon area (rs3135506 and rs2075291) are more likely to be linked to MetS susceptibility. APOA5 which function as a ligand for TG-rich lipoprotein, is a key regulator of plasma triglycerides. ApoA5 is a 366 amino acid protein primarily synthesized in hepatic cells and plays a vital role in lipid metabolism [61, 62]. Even though ApoA5 has low concentrations in the blood, its loss can impair lipoprotein lipase activity and cause an increase in TG levels [61, 62]. In addition, a lack of ApoA5 can disrupt the removal of remaining lipoproteins from the bloodstream, as it plays a role in assisting LDL receptors and heparan sulfate proteoglycans [61]. As a result, APOA5 polymorphism can lead to hypertrigiceridima which is proposed as a pivotal mechanism responsible for the increased susceptibility to MetS in relation to genetic variability at the APOA5 locus.
Although ApoA5 is not expressed in adipose tissue, it may still play a role in the accumulation of triglycerides in adipocytes [62]. The accumulation of TG in adipocytes can lead to a rise in resistin, TNF-α, and interleukin 6, which can result in insulin resistance [63]. Insulin resistance is the main notion behind MetS, and it may be responsible for the majority of its components [64].
Hypertension is another component of MetS that hypertriglyceridemia can influence it through some possible mechanisms, including disturbance of the vasodilation mechanisms leading to vascular resistance, stimulating aldosterone production, and inducing insulin resistance, which is caused by stimulation of the sympathetic nervous system activity and renin–angiotensin system [65,66,67,68]. APOA5 appears to be directly or indirectly involved in most MetS components and has an association with the development of MetS.
APOA5 deficiency can exert some influences on obesity, as an additional element of metabolic syndrome. Given that APOA1, APOC3, and APOA4 are genes associated with obesity and are grouped together in the same cluster as APOA5, it is possible that mutations in one gene within the cluster may be caused by genetic variations in another gene [69]. Furthermore, it can potentially reduce satiety-related signals and contribute to obesity as a result of consuming a large number of calories [70].
The HDL is another component of metabolic syndrome that might be affected by ApoA5 loss. The ApoA5 may affect HDL levels through TG metabolism, as there is a known negative link between triglyceride and HDL-C levels [71, 72]. Moreover, ApoA5 protein is a component of HDL particles, and its absence might result in unstable HDL that is easily eliminated from serum [72]. Furthermore, Apoa5 mutation can result in impaired reverse cholesterol transport and abnormal HDL maturation, resulting in a decrease in the total amount of HDL [73].
Implications from subgroup analyses
Our findings demonstrated that the rs662799 polymorphism is associated with metabolic syndrome (MetS) prevalence in both African and East Asian populations under the dominant model. The association observed in African populations should be interpreted with caution due to the limited number of studies (accounting for only 4% of the overall effect size). Previous meta-analysis have confirmed that APOA5 variants increase the risk of MetS in East Asian and non-white populations [23]. These discrepancies may be partially explained by factors such as differing gene-gene or gene-environment interactions [74], linkage disequilibrium patterns, and minor allele frequencies of the APOA5 SNPs [74, 75].
We also found a sex-specific association between the rs662799 polymorphism and MetS prevalence, with the association more evident in female participants. This association may be potentially justified by the fact that most female participants were in a post-menopausal status and did not benefit from exposure to female hormones, especially estrogen, which protects against visceral fat accumulation, insulin resistance, hypertension, and dyslipidemia [77].
The association between the rs662799 polymorphism and the prevalence of MetS is also influenced by the definition of MetS, with a stronger association observed when employing the IDF criteria. The IDF definition emphasizes central obesity and employed stricter cut-offs for specific MetS components, so the prevalence of MetS is typically higher when diagnosed using this definition than when using others [78].
Moreover, our results indicated that the associations of rs662799 and rs651821 with MetS were slightly stronger in the recessive models compared to the dominant models, indicating that wild-type alleles may be capable of partially attenuating the effect of mutant alleles in heterozygous individuals. Wu et al. concluded that the rs662799 and rs651821 variations are more closely linked to MetS when examined under a recessive genetic model than a dominant model [35]. It is suggested that if two copies of the allele at rs662799 or rs651821 are present, it may have a more significant effect on the risk of MetS [35]. Similarly, the results of other studies on rs662799 revealed that the concentration of ApoA5 in people with the C/C genotype is lower than that with the T/C and T/T genotypes, therefore, it is assumed that the recessive model has a higher risk of MetS than the dominant model [35, 79].
Future perspectives
It has been shown that different genes may be associated with the MetS developing, and some genes also reinforce each other’s effects [80]. Therefore, it is crucial to consider gene-gene interactions to obtain logical and reliable outcomes. Aside from the genetic component, environmental interactions, and epigenetic factors could play significant roles in the underlying mechanism of MetS [35, 81]. Therefore, future studies on the dysregulation of epigenetic factors in MetS would provide a deeper insight into MetS pathophysiology.
Strengths and limitations
The present meta-analysis has some strengths. This is the first comprehensive meta-analysis that investigates the majority of APOA5 polymorphisms associated with MetS and overcomes the constraints of prior meta-analyses. In addition, the results have been presented based on several subgroups in order to explore the source of heterogeneity and detect any variables that may affect the results of the meta-analysis. Nevertheless, our study, like other genetic meta-analyses, had several limitations that should be taken into account when interpreting the findings of the meta-analysis. Although we analysed the majority of the APOA5 SNPs, it is important to acknowledge that the potential effects of gene-gene interactions were not assessed in the current investigation and should not be disregarded. For example, the interactions between APOA5, BUD13, CETP, and LIPA have been reported to be involved in MetS susceptibility [82]. Aside from the genetic component, environmental and epigenetic factors could play important roles in MetS development [35, 83]. While our subgroup analysis examined the influence of some environmental variables (BMI, age, sex, smoking), the possibility of residual confounding due to unmeasured factors, such as diet or physical activity, cannot be excluded.
Another limitation was the limited number of eligible studies investigating rs651821, rs2075201, and rs126317 polymorphisms, which made it impossible to perform subgroup analysis for these variants.
Conclusion
We found that polymorphisms located in the promotor and codon regions of the APOA5 gene, including rs662799, rs3135506, rs651821, and rs2075291, were associated with increased MetS prevalence. However, because the sample size was small and there was evidence of significant heterogeneity for some APOA5 gene polymorphisms, these results need to be confirmed by more large-scale and well-designed studies.
Data availability
The datasets used or analysed during the current study are available from the corresponding author on reasonable request.
Abbreviations
- AHA/NHLBI:
-
American Heart Association/National Heart, Lung and Blood Institute
- APOA5:
-
Apolipoprotein A5
- APOC3:
-
Apolipoprotein C3
- ATP III (NCEP ATP III):
-
National Cholesterol Education Programme Adult Treatment Panel III
- BMI:
-
Body Mass Index
- CETP:
-
Cholesteryl Ester Transfer Protein
- CI:
-
Confidence Interval
- DNA:
-
Deoxyribonucleic Acid
- IDF:
-
International Diabetes Federation
- HDL:
-
High-density Lipoprotein
- HDL-C:
-
High-Density Lipoprotein Cholesterol
- HWE:
-
Hardy-Weinberg Equilibrium
- I2 :
-
I-squared
- JIS:
-
Joint Interim Statement
- LDL:
-
Low-density Lipoprotein
- LIPA:
-
Lipase A Lysosomal Acid type
- LPL:
-
Lipoprotein Lipase
- MetS:
-
Metabolic Syndrome
- MALDI-TOF:
-
Matrix-Assisted Laser Desorption/Ionization
- NOS:
-
Newcastle?Ottawa Scale
- OR:
-
Odd Ratio
- PCR-RFLP:
-
Polymerase Chain Reaction -Amplification Refractory Mutation System
- PCR-SSOP:
-
Polymerase Chain Reaction -Sequence Specific Oligonucleotide Probes
- p-value:
-
Probability value
- PRISMA:
-
Preferred Reporting Items for Systematic Reviews and Meta-Analyses
- SNP:
-
Single-Nucleotide Polymorphism
- SNP-IT:
-
SNP Integration Tool
- TG:
-
Triglyceride
- TNF-α:
-
The Role of Tumor Necrosis Factor Alpha
- TRL:
-
Triglyceride-rich Lipoprotein
- VLDL:
-
Very Low Density Lipoprotein
References
Xu H, Li X, Adams H, Kubena K, Guo S. Etiology of metabolic syndrome and dietary intervention. IJMS. 2018;20(1):128.
Noubiap JJ, Nansseu JR, Lontchi-Yimagou E, Nkeck JR, Nyaga UF, Ngouo AT, et al. Geographic distribution of metabolic syndrome and its components in the general adult population: a meta-analysis of global data from 28 million individuals. Diabetes Res Clin Pract. 2022;188:109924.
Alshammary AF, Alharbi KK, Alshehri NJ, Vennu V, Ali Khan I. Metabolic syndrome and coronary artery Disease Risk: a Meta-analysis of Observational studies. Int J Environ Res Public Health. 2021;18(4).
Ju SY, Lee JY, Kim DH. Association of metabolic syndrome and its components with all-cause and cardiovascular mortality in the elderly: a meta-analysis of prospective cohort studies. Medicine. 2017;96(45):e8491.
Zhong L, Liu J, Liu S, Tan G. Correlation between pancreatic cancer and metabolic syndrome: a systematic review and meta-analysis. Front Endocrinol. 2023;14:1116582.
Chen Z, Liu Z, Yang H, Liu C, Kong F. Metabolic syndrome and risk of ovarian cancer: a systematic review and meta-analysis. Front Endocrinol. 2023;14:1219827.
Lu B, Qian JM, Li JN. The metabolic syndrome and its components as prognostic factors in colorectal cancer: a meta-analysis and systematic review. J Gastroenterol Hepatol. 2023;38(2):187–96.
Esposito K, Chiodini P, Colao A, Lenzi A, Giugliano D. Metabolic syndrome and risk of cancer: a systematic review and meta-analysis. Diabetes Care. 2012;35(11):2402–11.
Mohamed SM, Shalaby MA, El-Shiekh RA, El-Banna HA, Emam SR, Bakr AF. Metabolic syndrome: risk factors, diagnosis, pathogenesis, and management with natural approaches. Food Chem Adv. 2023;3:100335.
Abdul Samad F, Suliman BA, Basha SH, Manivasagam T, Essa MM. A comprehensive in Silico analysis on the structural and functional impact of SNPs in the congenital heart defects associated with NKX2-5 gene—A molecular dynamic simulation approach. PLoS ONE. 2016;11(5):e0153999.
Yamada Y, Kato K, Hibino T, Yokoi K, Matsuo H, Segawa T, et al. Prediction of genetic risk for metabolic syndrome. Atherosclerosis. 2007;191(2):298–304.
Oh S-W, Lee J-E, Shin E, Kwon H, Choe EK, Choi S-Y, et al. Genome-wide association study of metabolic syndrome in Korean populations. PLoS ONE. 2020;15(1):e0227357.
Kraja AT, Vaidya D, Pankow JS, Goodarzi MO, Assimes TL, Kullo IJ, et al. A bivariate genome-wide approach to metabolic syndrome: STAMPEED consortium. Diabetes. 2011;60(4):1329–39.
Zhu Y, Zhang D, Zhou D, Li Z, Li Z, Fang L, et al. Susceptibility loci for metabolic syndrome and metabolic components identified in Han Chinese: a multi-stage genome-wide association study. J Cell Mol Med. 2017;21(6):1106–16.
Zafar U, Khaliq S, Lone KP. Genetic association of apolipoprotein A5-1131T > C polymorphism with traits of metabolic syndrome. J Coll Physicians Surg Pak. 2019;29(7):626–30.
Srivastava RK, Singh P, Verma P, Sethi R, Verma A, Ali W, et al. Influence of APOA5 (rs662799 and rs3135506) gene polymorphism in acute myocardial infarction patients and its association with basic coronary artery disease risk factors. J Appl Pharm Sci. 2015;5(6):008–14.
Su X, Kong Y, Peng D-q. New insights into apolipoprotein A5 in controlling lipoprotein metabolism in obesity and the metabolic syndrome patients. Lipids Health Dis. 2018;17(1):1–10.
Pennacchio LA, Olivier M, Hubacek JA, Cohen JC, Cox DR, Fruchart J-C, et al. An apolipoprotein influencing triglycerides in humans and mice revealed by comparative sequencing. Science. 2001;294(5540):169–73.
Ajjemami M, Ouatou S, Charoute H, Fakiri M, Rhaissi H, Benrahma H, et al. Haplotype analysis of the apolipoprotein A5 gene in Moroccan patients with the metabolic syndrome. J Diabetes Metab Disord. 2015;14:1–8.
Halalkhor S, Jalali F, Tilaki KH, Shojaei S. Association of two common polymorphisms of apolipoprotein A5 gene with metabolic syndrome indicators in a north Iranian population, a cross-sectional study. J Diabetes Metab Disord. 2014;13:1–7.
Kefi R, Hechmi M, Dallali H, Elouej S, Jmel H, Halima YB, et al. editors. Association of apolipoprotein A5 gene variants with metabolic syndrome in Tunisian population. Ann Endocrinol: Elsevier; 2017.
Kim YR, Hong S-H. Association of apolipoprotein A5 gene polymorphisms with metabolic syndrome in the Korean population. Genetic Test Mol Biomarkers. 2016;20(3):130–6.
Liu C-F, Yang Q-F, Chen X-L, Liu C-Y. Apolipoprotein a5 gene polymorphism and risk for metabolic syndrome: a meta-analysis. Genet Test Mol. 2012;16(10):1241–5.
Xu C, Bai R, Zhang D, Li Z, Zhu H, Lai M, et al. Effects of APOA5 – 1131T > C (rs662799) on fasting plasma lipids and risk of metabolic syndrome: evidence from a case-control study in China and a meta-analysis. PLoS ONE. 2013;8(2):e56216.
Hechmi M, Dallali H, Gharbi M, Jmel H, Fassatoui M, Ben Halima Y et al. Association of rs662799 variant and APOA5 gene haplotypes with metabolic syndrome and its components: a meta-analysis in North Africa. Bioscirep. 2020;40(8).
Alipour N, Kazemnejad A, Akbarzadeh M, Eskandari F, Zahedi AS, Daneshpour MS. Regularized machine learning models for prediction of metabolic syndrome using GCKR, APOA5, and BUD13 gene variants: Tehran cardiometabolic genetic study. Cell J (Yakhteh). 2023;25(8):536.
de Luis DA, Izaola O, Primo D, Aller R. APOA5 variant rs662799, role in cardiovascular traits and serum adipokine levels in caucasian obese subjects. ANN NUTR METAB. 2021;77(5):299–306.
Fathy MM, Wahab AA-A, Tabozada S, Ibrahim M, Aref W, Hamid MA-A. Association of apolipoprotein A5 gene 1131T/C polymorphism with dyslipidemia and insulin resistance in Egyptian patients with metabolic syndrome. Comp Clin Path. 2013;22:1245–50.
Fiaz M, Shaiq PA, Raj GK, Saqlain M, Mehmood A, Naqvi SMS, et al. Association study of apolipoprotein A5 gene (APOA5 gene) variant with the metabolic syndrome in local Pakistani population. J Pak Med Assoc. 2019;69(3):301–5.
Hiramatsu M, Oguri M, Kato K, Horibe H, Fujimaki T, Watanabe S, et al. Synergistic effects of genetic variants of APOA5 and BTN2A1 on dyslipidemia or metabolic syndrome. Int J Mol Med. 2012;30(1):185–92.
Kim DH, Lee SH, Han KH, Kim CB, Song KY, Cho S, et al. APOA5 polymorphism is associated with metabolic syndrome in Korean postmenopausal women. EnM. 2012;27(4):276–81.
Lim HH, Choi M, Kim JY, Lee JH, Kim OY. Increased risk of obesity related to total energy intake with the APOA5-1131T > C polymorphism in Korean premenopausal women. Nutr Res. 2014;34(10):827–36.
Novotny D, Vaverkova H, Karasek D, Malina P. Genetic variants of apolipoprotein A5 T-1131 C and apolipoprotein E common polymorphisms and their relationship to features of metabolic syndrome in adult dyslipidemic patients. Clin Biochem. 2014;47(12):1015–21.
Song KH, Cha S, Yu S-G, Yu H, Oh SA, Kang N-S. Association of Apolipoprotein A5 Gene 1131T C Polymorphism with the Risk of Metabolic Syndrome in Korean Subjects. bmri. 2013;2013.
Wu Y, Yu Y, Zhao T, Wang S, Fu Y, Qi Y, et al. Interactions of environmental factors and APOA1-APOC3-APOA4-APOA5 gene cluster gene polymorphisms with metabolic syndrome. PLoS ONE. 2016;11(1):e0147946.
Yeh K-H, Lin C-H, Hsiao T-H, Lu T-P, editors. Genome-wide association study (GWAS) on metabolic syndrome in subjects with abdominal obesity in a Taiwanese population. 2020 IEEE International Conference on Bioinformatics and Biomedicine (BIBM); 2020: IEEE.
Moher D, Liberati A, Tetzlaff J, Altman DG, medicine PGJAoi. Preferred reporting items for systematic reviews and meta-analyses: the PRISMA statement. 2009;151(4):264–9.
Wells GA, Wells G, Shea B, Shea B, O’Connell D, Peterson J, et al. editors. The Newcastle-Ottawa Scale (NOS) for Assessing the Quality of Nonrandomised Studies in Meta-Analyses2014.
Lewis CM. Genetic association studies: design, analysis and interpretation. BIB. 2002;3(2):146–53.
Lee YH. Meta-analysis of genetic association studies. Ann Lab Med. 2015;35(3):283.
DerSimonian R, Laird N. Meta-analysis in clinical trials. Control Clin Trials. 1986;7(3):177–88.
Higgins JP, Thompson SG. Quantifying heterogeneity in a meta-analysis. Stat Med. 2002;21(11):1539–58.
Huedo-Medina TB, Sánchez-Meca J, Marín-Martínez F, Botella J. Assessing heterogeneity in meta-analysis: Q statistic or I² index? Psychol Methods. 2006;11(2):193.
Egger M, Smith GD, Schneider M, Minder C. Bias in meta-analysis detected by a simple, graphical test. BMJ. 1997;315(7109):629–34.
Begg CB, Mazumdar M. Operating characteristics of a rank correlation test for publication bias. Biometrics. 1994:1088 – 101.
Dallongeville J, Cottel D, Wagner A, Ducimetière P, Ruidavets J-B, Arveiler D, et al. The APOA5Trp19 allele is associated with metabolic syndrome via its association with plasma triglycerides. Bmcmedgenet. 2008;9(1):1–9.
Grallert H, Sedlmeier E-M, Huth C, Kolz M, Heid IM, Meisinger C, et al. APOA5 variants and metabolic syndrome in Caucasianss. JLR. 2007;48(12):2614–21.
He F, Xu X, Hu D, Ma S, Tang L, Fan W, et al. Apolipoprotein A5-12238 T > C gene polymorphism and risk factors for metabolic syndrome in the Guo Shan Yao and the Han populations. CCLM. 2011;49(10):1755–7.
Hsu L-A, Ko Y-L, Chang C-J, Teng M-S, Wu S, Hu C-F. Apolipoprotein A5 gene – 1131T/C polymorphism is associated with the risk of metabolic syndrome in ethnic Chinese in Taiwan. CCLM. 2008;46(12):1714–9.
Kisfali P, Mohás M, Maász A, Polgar N, Hadarits F, Markó L, et al. Haplotype analysis of the apolipoprotein A5 gene in patients with the metabolic syndrome. NMCD. 2010;20(7):505–11.
Komurcu-Bayrak E, Onat A, Poda M, Humphries SE, Palmen J, Guclu F, et al. Gender-modulated impact of apolipoprotein A5 gene (APOA5) – 1131T > C and c. 56C > G polymorphisms on lipids, dyslipidemia and metabolic syndrome in Turkish adults. CCLM. 2008;46(6):778–84.
Lim MY, You HJ, Yoon HS, Kwon B, Lee JY, Lee S, et al. The effect of heritability and host genetics on the gut microbiota and metabolic syndrome. Gut. 2017;66(6):1031–8.
Mattei J, Demissie S, Tucker KL, Ordovas JM. Apolipoprotein A5 polymorphisms interact with total dietary fat intake in association with markers of metabolic syndrome in Puerto Rican older adults. J Nutr. 2009;139(12):2301–8.
Niculescu LS, Fruchart-Najib J, Fruchart J-C, Sima A. Apolipoprotein AV gene polymorphisms in subjects with metabolic syndrome. 2007.
Ong KL, Jiang CQ, Liu B, Jin YL, Tso AW, Tam S, et al. Association of a genetic variant in the apolipoprotein A5 gene with the metabolic syndrome in Chinese. Clin Endocrinol. 2011;74(2):206–13.
Vasilopoulos Y, Sarafidou T, Bagiatis V, Skriapa L, Goutzelas Y, Pervanidou P, et al. Association between polymorphisms in MTHFR and APOA5 and metabolic syndrome in the Greek population. Genet Test Mol. 2011;15(9):613–7.
Yamada Y, Kato K, Yoshida T, Yokoi K, Matsuo H, Watanabe S et al. Genetic risk for metabolic syndrome: examination of candidate gene polymorphisms related to lipid metabolism in Japanese individuals. J Med Genet. 2007.
Flores-Viveros KL, Aguilar-Galarza BA, Ordóñez-Sánchez ML, Anaya-Loyola MA, Moreno-Celis U, Vázquez-Cárdenas P, et al. Contribution of genetic, biochemical and environmental factors on insulin resistance and obesity in Mexican young adults. ORCP. 2019;13(6):533–40.
Masjoudi S, Sedaghati-Khayat B, Givi NJ, Bonab LNH, Azizi F, Daneshpour MS. Kernel machine SNP set analysis finds the association of BUD13, ZPR1, and APOA5 variants with metabolic syndrome in Tehran Cardio-metabolic Genetics Study. srep. 2021;11(1):10305.
Son KY, Son H-Y, Chae J, Hwang J, Jang S, Yun JM, et al. Genetic association of APOA5 and APOE with metabolic syndrome and their interaction with health-related behavior in Korean men. Lipids Health Dis. 2015;14(1):1–9.
Vrablik M, Hubacek JA, Dlouha D, Satny M, Adamkova V, Ceska R. Strong association between APOA5 gene polymorphisms and hypertriglyceridaemic episodes. Folia Biol (Praha). 2019;65(4):188–94.
Guardiola M, Ribalta J. Update on APOA5 Genetics: toward a better understanding of its physiological impact. Curr Atheroscler Rep. 2017;19(7):30.
Zhao J, Zhang Y, Wei F, Song J, Cao Z, Chen C, et al. Triglyceride is an independent predictor of type 2 diabetes among middle-aged and older adults: a prospective study with 8-year follow-ups in two cohorts. J Transl Med. 2019;17(1):403.
Beshara A, Cohen E, Goldberg E, Lilos P, Garty M, Krause I. Triglyceride levels and risk of type 2 diabetes mellitus: a longitudinal large study. J Investig Med. 2016;64(2):383–7.
Xing Y, Rainey WE, Apolzan JW, Francone OL, Harris RB, Bollag WB. Adrenal cell aldosterone production is stimulated by very-low-density lipoprotein (VLDL). Endocrinology. 2012;153(2):721–31.
Manrique C, Lastra G, Gardner M, Sowers JR. The renin angiotensin aldosterone system in hypertension: roles of insulin resistance and oxidative stress. Med Clin N Am. 2009;93(3):569–82.
Wang H, Zhou T, He H, Peng R, Wang S, Jiang X. APOA5 rs651821 confers increased risk for hypertension in Tongdao Dong population. Clin Exp Hypertens. 2020;42(1):81–5.
Ouatou S, Ajjemami M, Charoute H, Sefri H, Ghalim N, Rhaissi H, et al. Association of APOA5 rs662799 and rs3135506 polymorphisms with arterial hypertension in Moroccan patients. Lipids Health Dis. 2014;13:1–9.
Zhu WF, Wang CL, Liang L, Shen Z, Fu JF, Liu PN, et al. Triglyceride-raising APOA5 genetic variants are associated with obesity and non-HDL-C in Chinese children and adolescents. Lipids Health Dis. 2014;13:93.
Lim HH, Choi M, Kim JY, Lee JH, Kim OY. Increased risk of obesity related to total energy intake with the APOA5-1131T > C polymorphism in Korean premenopausal women. Nutr Res. 2014;34(10):827-36.
Lee KW, Ayyobi AF, Frohlich JJ, Hill JS. APOA5 gene polymorphism modulates levels of triglyceride, HDL cholesterol and FERHDL but is not a risk factor for coronary artery disease. Atherosclerosis. 2004;176(1):165–72.
Priore Oliva C, Carubbi F, Schaap FG, Bertolini S, Calandra S. Hypertriglyceridaemia and low plasma HDL in a patient with apolipoprotein A-V deficiency due to a novel mutation in the APOA5 gene. J Intern Med. 2008;263(4):450–8.
Long S, Chen Z, Han Y, Christopher DM, Zhang C, Yang Y, et al. Relationship between the distribution of plasma HDL subclasses and the polymorphisms of APOA5 in hypertriglyceridemia. Clin Biochem. 2013;46(9):733–9.
Cho YS, Go MJ, Kim YJ, Heo JY, Oh JH, Ban H-J, et al. A large-scale genome-wide association study of Asian populations uncovers genetic factors influencing eight quantitative traits. Nat Genet. 2009;41(5):527–34.
Lai CQ, Tai ES, Tan CE, Cutter J, Chew SK, Zhu YP, et al. The APOA5 locus is a strong determinant of plasma triglyceride concentrations across ethnic groups in Singapore. J Lipid Res. 2003;44(12):2365–73.
Chien KL, Fang WH, Wen HC, Lin HP, Lin YL, Lin SW et al. APOA1/C3/A5 haplotype and risk of hypertriglyceridemia in Taiwanese. Clinica chimica acta; international journal of clinical chemistry. 2008;390(1–2):56–62.
De Paoli M, Zakharia A, Werstuck GH. The role of estrogen in insulin resistance: a review of clinical and preclinical data. Am J Pathol. 2021;191(9):1490–8.
Gundogan K, Bayram F, Gedik V, Kaya A, Karaman A, Demir Ö, et al. Metabolic syndrome prevalence according to ATP III and IDF criteria and related factors in Turkish adults. Archives Med Sci. 2013;9(2):243–53.
Jang Y, Paik JK, Hyun YJ, Chae JS, Kim JY, Choi JR, et al. The apolipoprotein A5-1131T > C promoter polymorphism in koreans: association with plasma APOA5 and serum triglyceride concentrations, LDL particle size and coronary artery disease. Clin Chim Acta. 2009;402(1–2):83–7.
Dai W, Zhang Z, Yao C, Zhao S. Emerging evidences for the opposite role of apolipoprotein C3 and apolipoprotein A5 in lipid metabolism and coronary artery disease. Lipids Health Dis. 2019;18:1–7.
Guardiola M, Ribalta J. Update on APOA5 genetics: toward a better understanding of its physiological impact. Curr Atheroscler Rep. 2017;19:1–9.
Lin E, Kuo P-H, Liu Y-L, Yang AC, Kao C-F, Tsai S-J. Association and interaction of APOA5, BUD13, CETP, LIPA and health-related behavior with metabolic syndrome in a Taiwanese population. Sci Rep. 2016;6(1):1–9.
Stančáková A, Laakso M. Genetics of metabolic syndrome. Rev Endocr Metab Disord. 2014;15:243–52.
Acknowledgements
We would like to acknowledge the digital Library of clinical development center of Afshar hospital for giving us the opportunity to search electronic databases.
Funding
This work was supported by the Shahid Sadoughi University of Medical Sciences, Yazd, Iran. The funding source played no role in study design; in the collection, analysis, and interpretation of data; in the writing of the report; or in the decision to submit the article for publication.
Author information
Authors and Affiliations
Contributions
SS, and SM: Study conception and design SS, and SM: Search strategy preparation SM, SMEM: Data extraction SS: Analysis and interpretation of results RS, and SRM: Quality assessment SS, SM, MA, SMEM, and ADF: Draft manuscript preparation.
Corresponding author
Ethics declarations
Ethics approval and consent to participate
All data and analyses in this research were based on previous published studies, thus ethical approval and patient consent are not applicable for it.
Consent for publication
Not applicable.
Competing interests
The authors declare no competing interests.
Additional information
Publisher’s Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Electronic supplementary material
Below is the link to the electronic supplementary material.
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.
About this article
Cite this article
Mozafari, S., Ashoori, M., Emami Meybodi, S.M. et al. Association between APOA5 polymorphisms and susceptibility to metabolic syndrome: a systematic review and meta-analysis. BMC Genomics 25, 590 (2024). https://0-doi-org.brum.beds.ac.uk/10.1186/s12864-024-10493-x
Received:
Accepted:
Published:
DOI: https://0-doi-org.brum.beds.ac.uk/10.1186/s12864-024-10493-x