PPAR-γ2 and PTPRD gene polymorphisms influence type 2 diabetes patients' response to pioglitazone in China

Pei, Qi; Huang, Qiong; Yang, Gaoyi; Zhao, Ying; Yin, Ji‐Ye; Song, Min Seob; Zheng, Yi; Mo, Zhao Hui; Zhou, Hong; Liu, Zhao‐Qian

doi:10.1038/aps.2012.144

Cited by 50 publications

(40 citation statements)

References 38 publications

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“…This study also indicated that P12A mutation might also be linked to adipogenesis [66]. Furthermore, various research groups have shown that biological variability linked with the glucose-lowering effect of pioglitazone is also partly ascribed to the polymorphism associated with PPARG gene [67–69]. The PTPRD SNP rs17584499, located in intron 10, has been identified in Chinese populations as another important factor leading to pharmacodynamic variability in the glucose-lowering effect of pioglitazone [69].…”

Section: Pharmacogenomics and Pharmacogenetics Of Pioglitazone In Diabetesmentioning

confidence: 97%

“…Furthermore, various research groups have shown that biological variability linked with the glucose-lowering effect of pioglitazone is also partly ascribed to the polymorphism associated with PPARG gene [67–69]. The PTPRD SNP rs17584499, located in intron 10, has been identified in Chinese populations as another important factor leading to pharmacodynamic variability in the glucose-lowering effect of pioglitazone [69]. A substantial alteration of pioglitazone-induced reduction in HbAlc was observed in ADIPOQ C-11377G genotype and ADIPOR2 G795A genotype in Chinese and Iranian T2D populations [43,70].…”

Section: Pharmacogenomics and Pharmacogenetics Of Pioglitazone In Diabetesmentioning

confidence: 99%

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Pharmacogenomics and Pharmacogenetics of Thiazolidinediones: Role in Diabetes and Cardiovascular Risk Factors

et al. 2014

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The most important goal in the treatment of patients with diabetes is to prevent the risk of cardiovascular disease (CVD), the first cause of mortality in these subjects. Thiazolidinediones (TZDs), a class of antidiabetic drugs, act as insulin sensitizers increasing insulin-dependent glucose disposal and reducing hepatic glucose output. TZDs including pioglitazone, rosiglitazone and troglitazone, by activating PPAR-γ have shown pleiotropic effects in reducing vascular risk factors and atherosclerosis. However, troglitazone was removed from the market due to its hepatoxicity, and rosiglitazone and pioglitazone both have particular warnings due to being associated with heart diseases. Specific genetic variations in genes involved in the pathways regulated by TDZs have demonstrated to modify the variability in treatment with these drugs, especially in their side effects. Therefore, pharmacogenomics and pharmacogenetics are an important tool in further understand intersubject variability per se but also to assess the therapeutic potential of such variability in drug individualization and therapeutic optimization.

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Section: Pharmacogenomics and Pharmacogenetics Of Pioglitazone In Diabetesmentioning

confidence: 97%

Section: Pharmacogenomics and Pharmacogenetics Of Pioglitazone In Diabetesmentioning

confidence: 99%

Pharmacogenomics and Pharmacogenetics of Thiazolidinediones: Role in Diabetes and Cardiovascular Risk Factors

et al. 2014

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“…In 197 Chinese Han T2DM patients of whom 67 patients were given pioglitazone (30 mg/day for 12 weeks), those patients with PPARγ2 gene polymorphism rs1801282 CG showed significantly higher levels of PPPG and serum triglyceride compared with those with rs1801282 CC genotype 28. In patients with protein tyrosine phosphatase receptor type D gene polymorphism rs17584499, the CC genotype had better PPPG levels compared with CT + TT genotypes 28.…”

Section: Thiazolidinedionesmentioning

confidence: 99%

“…In patients with protein tyrosine phosphatase receptor type D gene polymorphism rs17584499, the CC genotype had better PPPG levels compared with CT + TT genotypes 28. In 241 Chinese patients with T2DM of whom 41 patients were given rosiglitazone (4 mg daily for 12 weeks), the presence of the SNPs Thr394Thr and Gly482Ser of the PPARγ coactivator-1 gene increased the therapeutic efficacy of rosiglitazone when compared to controls 29…”

Section: Thiazolidinedionesmentioning

confidence: 99%

Patient profiling in diabetes and role of canagliflozin

Amblee

2014

PGPM

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Genome-wide association studies have opened the door for patient profiling and research into genetic variants in multifactorial T2DM. Clinically, it may be possible to tailor the type of medication used based on the presence or absence of the various genetic variants. However, the polymorphisms studied may only explain some of the variability in response to T2DM drugs and needs further validation to ensure its authenticity. There are still unidentified factors which appear to play a role in the interindividual variability seen in clinical practice. The potential exists for pharmacogenomics to promote efficacious, safe, and cost-effective individualized diabetes management. Pharmacogenomics is still in its early stages, and the idea of defining patients genetically to predict individual responses to drugs and obtain safe and effective T2DM management is promising, in spite of existing barriers. Currently, clinical profiling of patients with T2DM and using an individualized approach with most drugs, including canagliflozin, based on comorbid conditions still remains the most accepted approach for the management of T2DM.

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“…Interestingly, in this study rs17584499 was found to be associated also with pioglitazone therapeutic efficacy. In fact, patients with rs17584499 CT+TT genotypes showed significantly lower differential value of postprandial plasma glucose compared to those with CC genotype after pioglitazone treatment for 3 months [58]. …”

Section: Ptprf and R2a Ptp Subfamilymentioning

confidence: 99%

Variants of Insulin-Signaling Inhibitor Genes in Type 2 Diabetes and Related Metabolic Abnormalities

Lorenzo

Greco

Fiorentino

et al. 2013

International Journal of Genomics

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Insulin resistance has a central role in the pathogenesis of several metabolic diseases, including type 2 diabetes, obesity, glucose intolerance, metabolic syndrome, atherosclerosis, and cardiovascular diseases. Insulin resistance and related traits are likely to be caused by abnormalities in the genes encoding for proteins involved in the composite network of insulin-signaling; in this review we have focused our attention on genetic variants of insulin-signaling inhibitor molecules. These proteins interfere with different steps in insulin-signaling: ENPP1/PC-1 and the phosphatases PTP1B and PTPRF/LAR inhibit the insulin receptor activation; INPPL1/SHIP-2 hydrolyzes PI3-kinase products, hampering the phosphoinositide-mediated downstream signaling; and TRIB3 binds the serine-threonine kinase Akt, reducing its phosphorylation levels. While several variants have been described over the years for all these genes, solid evidence of an association with type 2 diabetes and related diseases seems to exist only for rs1044498 of the ENPP1 gene and for rs2295490 of the TRIB3 gene. However, overall the data recapitulated in this Review article may supply useful elements to interpret the results of novel, more technically advanced genetic studies; indeed it is becoming increasingly evident that genetic information on metabolic diseases should be interpreted taking into account the complex biological pathways underlying their pathogenesis.

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PPAR-γ2 and PTPRD gene polymorphisms influence type 2 diabetes patients' response to pioglitazone in China

Cited by 50 publications

References 38 publications

Pharmacogenomics and Pharmacogenetics of Thiazolidinediones: Role in Diabetes and Cardiovascular Risk Factors

Pharmacogenomics and Pharmacogenetics of Thiazolidinediones: Role in Diabetes and Cardiovascular Risk Factors

Patient profiling in diabetes and role of canagliflozin

Variants of Insulin-Signaling Inhibitor Genes in Type 2 Diabetes and Related Metabolic Abnormalities

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