Department of Pediatrics, Comer Children's Hospital, The University of Chicago, Chicago, IL, USA.
Lipids Health Dis. 2010 Feb 15;9:18. doi: 10.1186/1476-511X-9-18.
Obesity increases the risk for insulin resistance and metabolic syndrome in both adults and children. FABP4 is a member of the intracellular lipid-binding protein family that is predominantly expressed in adipose tissue, and plays an important role in maintaining glucose and lipid homeostasis. The purpose of this study was to measure FABP4 plasma levels, assess FABP4 allelic variants, and explore potential associations with fasting glucose and insulin levels in young school-age children with and without obesity.
A total of 309 consecutive children ages 5-7 years were recruited. Children were divided based on BMI z score into Obese (OB; BMI z score >1.65) and non-obese (NOB). Fasting plasma glucose, lipids, insulin, hsCRP, and FABP4 levels were measured. HOMA was used as correlate of insulin sensitivity. Four SNPs of the human FABP4 gene (rs1051231, rs2303519, rs16909233 and rs1054135), corresponding to several critical regions of the encoding FABP4 gene sequence were genotyped.
Compared to NOB, circulating FABP4 levels were increased in OB, as were LDL, hsCRP and HOMA. FABP4 levels correlated with BMI, and also contributed to the variance of HOMA and hsCRP, but not serum lipids. The frequency of rs1054135 allelic variant was increased in OB, and was associated with increased FABP4 levels, while the presence of rs16909233 variant allele, although similar in OB and NOB, was associated with increased HOMA values.
Childhood obesity is associated with higher FABP4 levels that may promote cardiometabolic risk. The presence of selective SNPs in the FABP4 gene may account for increased risk for insulin resistance or systemic inflammation in the context of obesity.
肥胖症会增加成年人和儿童患胰岛素抵抗和代谢综合征的风险。FABP4 是细胞内脂质结合蛋白家族的成员,主要在脂肪组织中表达,在维持葡萄糖和脂质内稳态方面发挥着重要作用。本研究旨在测量 FABP4 血浆水平,评估 FABP4 等位基因变异,并探讨其与肥胖和非肥胖的年轻学龄儿童空腹血糖和胰岛素水平之间的潜在关联。
共招募了 309 名连续的 5-7 岁儿童。根据 BMI z 评分将儿童分为肥胖组(OB;BMI z 评分>1.65)和非肥胖组(NOB)。测量空腹血糖、血脂、胰岛素、hsCRP 和 FABP4 水平。HOMA 用于评估胰岛素敏感性。人类 FABP4 基因的 4 个 SNP(rs1051231、rs2303519、rs16909233 和 rs1054135),对应于编码 FABP4 基因序列的几个关键区域,进行了基因分型。
与 NOB 相比,OB 组循环 FABP4 水平升高,LDL、hsCRP 和 HOMA 也升高。FABP4 水平与 BMI 相关,并且可以解释 HOMA 和 hsCRP 的差异,但不能解释血脂的差异。OB 组 rs1054135 等位基因变异的频率增加,与 FABP4 水平升高相关,而 rs16909233 等位基因变异的存在虽然在 OB 和 NOB 中相似,但与 HOMA 值升高相关。
儿童肥胖与更高的 FABP4 水平相关,这可能会增加心血管代谢风险。FABP4 基因中的选择性 SNP 的存在可能会导致肥胖人群中胰岛素抵抗或全身炎症的风险增加。