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Effects of circulating member B of the family with sequence similarity 3 on the risk of developing metabolic syndrome and its components: A 5‐year prospective study

机译:具有序列相似性3的家庭循环成员B对发生代谢综合征及其组成部分的风险的影响:一项为期5年的前瞻性研究

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Aims/Introduction Member B of the family with sequence similarity 3 (FAM3B), also known as pancreatic‐derived factor, is mainly synthesized and secreted by islet β‐cells, and plays a role in abnormal metabolism of glucose and lipids. However, the prospective association of FAM3B with metabolic disorders remains unclear. The present study aimed to reveal the predictive relationship between pancreas‐specific cytokine and metabolic syndrome (MetS). Materials and Methods A total of 210 adults (88 men and 122 women) without MetS, aged between 40 and 65 years, were recruited and received a comprehensive health examination. Baseline serum FAM3B levels were determined by sandwich enzyme‐linked immunosorbent assay. Subsequently, all participants underwent a follow‐up examination after 5 years. MetS was identified in accordance with the International Diabetes Federation criteria. Results During follow up, 35.7% participants developed MetS. In comparison with the non‐MetS group, participants with MetS had an increased serum FAM3B at baseline (21.85 ng/mL [19.38, 24.17 ng/mL] vs 28.56 ng/mL [25.32, 38.10 ng/mL], P Conclusions Elevated circulating FAM3B might be considered as a predictor of newly‐onset MetS and its progression.
机译:目的/简介具有序列相似性3(FAM3B)的家族成员B,也称为胰腺衍生因子,主要由胰岛β细胞合成和分泌,在葡萄糖和脂质的异常代谢中起作用。然而,FAM3B与代谢紊乱的前瞻性关联仍不清楚。本研究旨在揭示胰腺特异性细胞因子与代谢综合征(MetS)之间的预测关系。材料和方法总共招募了210名无MetS的成年人(88名男性和122名女性),年龄在40至65岁之间,并接受了全面的健康检查。基线血清FAM3B水平通过夹心酶联免疫吸附试验测定。随后,所有参与者均在5年后接受了随访检查。 MetS是根据国际糖尿病联合会的标准确定的。结果随访期间,有35.7%的参与者制定了MetS。与非MetS组相比,MetS受试者的基线血清FAM3B升高(21.85 ng / mL [19.38,24.17 ng / mL]与28.56 ng / mL [25.32,38.10 ng / mL],P)结论循环升高FAM3B可能被认为是新发MetS及其进展的预测因子。

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