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11482G>A 多态性与饮食摄入相互作用,调节正常体重肥胖综合征成年人的人体测量指标和血脂谱。

Polymorphism 11482 G>A interacts with dietary intake to modulate anthropometric measures and lipid profile in adults with normal-weight obesity syndrome.

机构信息

Nutrition Undergraduate Course, Federal University of Tocantins, Quadra 109 Norte, Av. NS-15, Alcno-14, Bloco Bala I, Plano Diretor Norte, Palmas, TO, 77001-090, Brazil.

Nutritional Genomics Research Group, School of Nutrition, Federal University of Goiás, Rua 227, Quadra 68, s/n. Setor Leste Universitário, Goiânia, GO, 74.605-080, Brazil.

出版信息

Br J Nutr. 2022 Sep 28;128(6):1004-1012. doi: 10.1017/S0007114521004396. Epub 2021 Nov 2.

DOI:10.1017/S0007114521004396
PMID:34725012
Abstract

Evidence shows that genetic polymorphisms in perilipin 1 gene () are associated with excessive accumulation of body fat and disturbances in cardiometabolic markers. Therefore, the aim of this study was to verify whether the SNP 11482 G>A (rs894160) interacts with nutrient intake, anthropometric, body composition and cardiometabolic markers in adults with normal-weight obesity (NWO) syndrome. A cross-sectional study was carried out with 116 individuals aged 20-59 years, with normal BMI and high percentage of body fat. Anthropometric and body composition measures, glycaemic control and serum lipid markers, SNP 11482 G>A and nutrient intake were evaluated. Interactions between nutrient intake and the SNP were determined by regression models and adjusted for potential confounders. The SNP frequency was 56·0 % GG, 38·8 % GA and 5·2 % AA. Anthropometric measures and biochemical markers were not different according to genotype, except for total cholesterol (TC), LDL-cholesterol and non-HDL-cholesterol concentrations. However, important interactions between the SNP and dietary intake were observed. Carbohydrate intake interacted with the SNP 11482 G>A to modulate waist circumference (WC) and the homeostatic model assessment of insulin resistance index. Interaction of lipid intake and the SNP modulated TC and LDL-cholesterol concentrations, and the interaction between protein intake and the SNP tended to modulate weight, WC and BMI. The SNP 11482 G>A seems to modulate responses in anthropometric and lipid profile biomarkers of subjects with NWO depending on the dietary macronutrient composition, which may have long-term impact on cardiometabolic markers.

摘要

证据表明, perilipin 1 基因 () 的遗传多态性与体脂肪过度积累和心脏代谢标志物紊乱有关。因此,本研究旨在验证 SNP 11482 G>A (rs894160) 是否与正常体重肥胖 (NWO) 综合征成年人的营养摄入、人体测量、身体成分和心脏代谢标志物相互作用。进行了一项横断面研究,共纳入 116 名年龄在 20-59 岁、BMI 正常但体脂肪百分比高的成年人。评估了人体测量和身体成分指标、血糖控制和血清脂质标志物、SNP 11482 G>A 和营养摄入。通过回归模型确定了营养摄入与 SNP 之间的相互作用,并对潜在混杂因素进行了调整。SNP 频率为 56.0% GG、38.8% GA 和 5.2% AA。除了总胆固醇 (TC)、LDL-胆固醇和非 HDL-胆固醇浓度外,基因型与人体测量和生化标志物无差异。然而,观察到 SNP 与饮食摄入之间存在重要的相互作用。碳水化合物摄入量与 SNP 11482 G>A 相互作用,调节腰围 (WC) 和稳态模型评估的胰岛素抵抗指数。脂质摄入量与 SNP 的相互作用调节 TC 和 LDL-胆固醇浓度,而蛋白质摄入量与 SNP 的相互作用则倾向于调节体重、WC 和 BMI。SNP 11482 G>A 似乎根据饮食中宏量营养素的组成,调节 NWO 患者的人体测量和脂质谱生物标志物的反应,这可能对心脏代谢标志物产生长期影响。

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