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The Correlation of Increased CRP Levels with NFKB1 and TLR2 Polymorphisms in the Case of Morbid Obesity
Authors:T Soydas  O Karaman  H Arkan  G Yenmis  M M Ilhan  K Tombulturk  E Tasan  G Kanigur Sultuybek
Institution:1. Department of Medical Biology, Cerrahpa?a Medical Faculty, Istanbul University, Istanbul, Turkey;2. Division of Endocrinology and Metabolism, Department of Internal Medicine, Bezmialem Medical Faculty, Bezmialem University, Istanbul, Turkey;3. Department of Endocrinology and Metabolism, Umraniye Training and Research Hospital, Umraniye, Istanbul, Turkey
Abstract:Morbid obesity (MO) is associated with an increase in circulating levels of systemic acute phase proteins such as C‐reactive protein (CRP). Toll‐like receptor is possible candidate for inflammatory responses which is mainly mediated by NFKB1. The aim of this study was to investigate the relationship between NFKB1 and Toll‐like receptor (TLR) 2 polymorphisms and the risk of MO in a Turkish population in the context of CRP serum levels which may contribute to susceptibility to the disease. We analysed the distribution of NFKB1‐94 ins/del ATTG rs28362491 and TLR2 Arg753Gln rs5743708 polymorphisms using PCR‐RFLP method and CRP serum levels using ELISA method in 213 MO and 200 healthy controls. The frequency of the ins/ins genotype and ins allele of rs28362491 was significantly higher in the patients compared to control group (P: 0.0309; P: 0.0421, respectively). Additionally, the frequency of GG genotype and G allele of rs5743708 was found to be statistically higher in the patient group (P: 0.0421; < 0.0001, respectively). In addition, serum CRP levels (>20 mg/l) in MO patients with ins/ins genotype were significantly higher than in patients with del/ins genotype (P: 0.0309). Serum CRP levels were also higher in MO patients with GG genotype and G allele (P: 0.0001). According to combined analysis, the wild type of rs28362491 and rs5743708 polymorphisms (ins/ins/GG genotype) was also significantly higher in the patient group versus the control group when compared with the combined ins/ins/GA and del/ins/GA genotype (< 0.0001). Therefore, our findings suggest that rs28362491 and rs5743708 polymorphisms were significantly associated with MO disease through acting by modulating serum CRP levels.
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