Haplotype-based interaction of the PPARGC1A and UCP1 genes is associated with impaired fasting glucose or type 2 diabetes mellitus

Pei, Xiaoting; Liu, Li; Cai, Jialin; Wei, Wenkai; Shen, Yan; Wang, Yaxuan; Chen, Yanzi; Sun, Panpan; Imam, Mustapha Umar; Ping, Zhiguang; Fu, Xiaoli

doi:10.1097/md.0000000000006941

Cited by 12 publications

(7 citation statements)

References 27 publications

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“…Phasing, also known as haplotype estimation, reconstructs the haplotype sequences from genotype data and has been essential for understanding sequence-specific variation such as allele-specific expression [4, 5], methylation effects [6], and compound heterozygosity [2, 7]. Moreover, numerous studies have shown that haplotype-based association analysis can identify variants that would be missed by a standard single nucleotide polymorphism (SNP)-based analysis [8–10].…”

Section: Introductionmentioning

confidence: 99%

Exploring effective approaches for haplotype block phasing

et al. 2019

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BackgroundKnowledge of phase, the specific allele sequence on each copy of homologous chromosomes, is increasingly recognized as critical for detecting certain classes of disease-associated mutations. One approach for detecting such mutations is through phased haplotype association analysis. While the accuracy of methods for phasing genotype data has been widely explored, there has been little attention given to phasing accuracy at haplotype block scale. Understanding the combined impact of the accuracy of phasing tool and the method used to determine haplotype blocks on the error rate within the determined blocks is essential to conduct accurate haplotype analyses.ResultsWe present a systematic study exploring the relationship between seven widely used phasing methods and two common methods for determining haplotype blocks. The evaluation focuses on the number of haplotype blocks that are incorrectly phased. Insights from these results are used to develop a haplotype estimator based on a consensus of three tools. The consensus estimator achieved the most accurate phasing in all applied tests. Individually, EAGLE2, BEAGLE and SHAPEIT2 alternate in being the best performing tool in different scenarios. Determining haplotype blocks based on linkage disequilibrium leads to more correctly phased blocks compared to a sliding window approach. We find that there is little difference between phasing sections of a genome (e.g. a gene) compared to phasing entire chromosomes. Finally, we show that the location of phasing error varies when the tools are applied to the same data several times, a finding that could be important for downstream analyses.ConclusionsThe choice of phasing and block determination algorithms and their interaction impacts the accuracy of phased haplotype blocks. This work provides guidance and evidence for the different design choices needed for analyses using haplotype blocks. The study highlights a number of issues that may have limited the replicability of previous haplotype analysis.

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Section: Introductionmentioning

confidence: 99%

Exploring effective approaches for haplotype block phasing

et al. 2019

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“…For instance, the frequency of AG genotype of A-3826G in persons with CMP ranges from 24% in Italy [ 25 ], to around 50% in Colombia [ 20 ], Japan [ 21 ], and Korea [ 17 ], and to 85% in China [ 19 ]. Similarly, wide frequency ranges have been reported also for the other three SNPs across different populations [ 10 , 20 , 26 , 27 ]. At the same time, some studies report that UCP1 SNPs are strongly associated with disease risk [ 7 , 19 , 28 ], while others report no such findings [ 29 – 31 ].…”

Section: Introductionmentioning

confidence: 57%

Prevalence of uncoupling protein one genetic polymorphisms and their relationship with cardiovascular and metabolic health

et al. 2022

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Contribution of UCP1 single nucleotide polymorphisms (SNPs) to susceptibility for cardiometabolic pathologies (CMP) and their involvement in specific risk factors for these conditions varies across populations. We tested whether UCP1 SNPs A-3826G, A-1766G, Ala64Thr and A-112C are associated with common CMP and their risk factors across Armenia, Greece, Poland, Russia and United Kingdom. This case-control study included genotyping of these SNPs, from 2,283 Caucasians. Results were extended via systematic review and meta-analysis. In Armenia, GA genotype and A allele of Ala64Thr displayed ~2-fold higher risk for CMP compared to GG genotype and G allele, respectively (p<0.05). In Greece, A allele of Ala64Thr decreased risk of CMP by 39%. Healthy individuals with A-3826G GG genotype and carriers of mutant allele of A-112C and Ala64Thr had higher body mass index compared to those carrying other alleles. In healthy Polish, higher waist-to-hip ratio (WHR) was observed in heterozygotes A-3826G compared to AA homozygotes. Heterozygosity of A-112C and Ala64Thr SNPs was related to lower WHR in CMP individuals compared to wild type homozygotes (p<0.05). Meta-analysis showed no statistically significant odds-ratios across our SNPs (p>0.05). Concluding, the studied SNPs could be associated with the most common CMP and their risk factors in some populations.

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“…For instance, the frequency of AG of A-3826G in persons with CMP ranges from 24% in Italy (22), to around 50% in Colombia (10), Japan (19), and Korea (16), and to 85% in China (18). Similarly wide frequency ranges have been reported also for the other three SNPs across different populations (11,(23)(24)(25). At the same time, some studies report that UCP1 SNPs are strongly associated with disease risk (9,18,26), while others report no such findings (27)(28)(29).…”

Section: Introductionmentioning

confidence: 78%

Prevalence of uncoupling protein one genetic polymorphisms and their relationship with cardiovascular and metabolic health

Nintou

Vliora

et al. 2021

Preprint

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The contribution of UCP1 single nucleotide polymorphisms (SNPs) to susceptibility for cardiometabolic pathologies (CMP) and their involvement in specific risk factors for these conditions varies across populations. We tested whether UCP1 SNPs A-3826G, A-1766G, Ala64Thr and A-112C are associated with the most common CMP (cardiovascular disease, hypertension, metabolic syndrome, and type-2 diabetes) and CMP risk factors. This case-control study included blood sample collection from 2,283 Caucasians (1,139 healthy; 1,144 CMP) across Armenia, Greece, Poland, Russia and United Kingdom for genotyping of the above-mentioned SNPs. We extended the results via a systematic review and meta-analysis, covering PubMed, Embase, and Cochrane Library databases. In Armenia the GA genotype and A allele of Ala64Thr were associated with ~2-fold higher risk for CMP compared to the GG genotype or G allele, respectively (p<0.05). In Greece, A allele of Ala64Thr SNP decreased the risk of CMP by 39%. Healthy individuals with A-3826G GG genotype and carriers of mutant allele of A-112C and Ala64Thr had higher body mass index compared to those carrying other genotypes. In healthy Polish, higher waist-to-hip ratio (WHR) was observed in heterozygotes A-3826G compared to AA homozygotes. Heterozygosity of the A-112C and Ala64Thr SNPs was related to lower WHR in CMP individuals compared to wild type homozygotes (p<0.05). Meta-analysis in case-control studies showed no statistically significant odds ratios in different alleles across the four studied SNPs (p>0.05). Thus, we conclude that the studied SNPs could be associated with the most common CMP and their risk factors in some populations.

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Haplotype-based interaction of the PPARGC1A and UCP1 genes is associated with impaired fasting glucose or type 2 diabetes mellitus

Cited by 12 publications

References 27 publications

Exploring effective approaches for haplotype block phasing

Exploring effective approaches for haplotype block phasing

Prevalence of uncoupling protein one genetic polymorphisms and their relationship with cardiovascular and metabolic health

Prevalence of uncoupling protein one genetic polymorphisms and their relationship with cardiovascular and metabolic health

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