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Ciprofibrate therapy in patients with hypertriglyceridemia and low high density lipoprotein (HDL)-cholesterol: greater reduction of non-HDL cholesterol in subjects with excess body weight (The CIPROAMLAT study)
Authors:Carlos A Aguilar-Salinas  Andréia Assis-Luores-Vale  Benjamín Stockins  Hector Mario Rengifo  Dondici José Filho  Abrahão Afiune Neto  Marcílio Lísia Rabelo  Kerginaldo Paulo Torres  Egídio Paulo de José Oliveira  Carlos Alberto Machado  Eliana Reyes  Victor Saavedra  Fernando Florenzano  Ma Victoria Hernández  Hernandez Sergio Jiménez  Erika Ramírez  Cuauhtémoc Vazquez  Saul Salinas  Ismael Hernández  Octavio Medel  Ricardo Moreno  Paula Lugo  Ricardo Alvarado  Roopa Mehta  Victor Gutierrez  Francisco J Gómez Pérez
Affiliation:1. Centre for Cardiovascular Genetics, British Heart Foundation Laboratories, Royal Free & University College London Medical School, 5 University Street, London, WC1E 6JF, United Kingdom
2. Department of Diabetes & Endocrinology, UCL Hospitals, Mortimer Street, London, W1T 3AA, United Kingdom
Abstract:

Background

Microalbuminuria and subsequent progression to proteinuria and nephropathy is associated with increased oxidative stress, increased inflammatory cytokines and increased cardiovascular (CVD) risk. The common functional IL-6 -174G>C gene variant is also associated with elevated levels of inflammatory cytokines and CVD risk.

Methods

The aim of this study was to examine the association between the IL-6 -174G>C gene variant with plasma total antioxidant status (TAOS) in 552 subjects with type 2 diabetes in relation to urinary protein excretion.

Results

In subjects free from CVD, there was a significant interaction between urinary protein excretion (normoalbuminuria/ microalbuminuria/proteinuria) and the -174C allele (compared to -174GG) in determining plasma TAOS (p value for interaction = 0.03). In the -174C allele carriers there was a significant association between plasma TAOS and urinary protein excretion: normalbuminuria v microalbuminuria v proteinuria: 44.30% ± 11.32 vs. 39.74% ± 14.83 vs. 37.93% ± 16.42, ANOVA p = 0.025. In those with CVD, no interaction or association was observed with the -174C allele (p = 0.246).

Conclusion

The IL-6 -174G>C gene variant is associated with differences in plasma oxidative stress in response to altered protein excretion in subjects with type 2 diabetes.
Keywords:
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