Weickert Martin O, Loeffelholz Christian V, Roden Michael, Chandramouli Visvanathan, Brehm Attila, Nowotny Peter, Osterhoff Martin A, Isken Frank, Spranger Jochen, Landau Bernard R, Pfeiffer Andreas F H, Möhlig Matthias
Dept. of Clinical Nutrition, German Institute of Human Nutrition Potsdam-Rehbruecke, Arthur-Scheunert-Allee 114-116, 14558 Nuthetal, Germany.
Am J Physiol Endocrinol Metab. 2007 Oct;293(4):E1078-84. doi: 10.1152/ajpendo.00337.2007. Epub 2007 Aug 14.
Liver fatty acid-binding protein (L-FABP) is a highly conserved key factor in lipid metabolism. Amino acid replacements in L-FABP might alter its function and thereby affect glucose metabolism in lipid-exposed subjects, as indicated by studies in L-FABP knockout mice. Amino acid replacements in L-FABP were investigated in a cohort of 1,453 Caucasian subjects. Endogenous glucose production (EGP), gluconeogenesis, and glycogenolysis were measured in healthy carriers of the only common Thr(94)-to-Ala amino acid replacement (Ala/Ala(94)) vs. age-, sex-, and BMI-matched wild-type (Thr/Thr(94)) controls at baseline and after 320-min lipid/heparin-somatostatin-insulin-glucagon clamps (n = 18). Whole body glucose disposal was further investigated (subset; n = 13) using euglycemic-hyperinsulinemic clamps without and with lipid/heparin infusion. In the entire cohort, the only common Ala/Ala(94) mutation was significantly associated with reduced body weight, which is in agreement with a previous report. In lipid-exposed, individually matched subjects there was a genotype vs. lipid-treatment interaction for EGP (P = 0.009) driven mainly by reduced glycogenolysis in Ala/Ala(94) carriers (0.46 +/- 0.05 vs. 0.59 +/- 0.05 mgxkg(-1)xmin(-1), P = 0.013). The lipid-induced elevation of plasma glucose levels was smaller in Ala/Ala(94) carriers compared with wild types (P < 0.0001). Whole body glucose disposal was not different between lipid-exposed L-FABP genotypes. In summary, the Ala/Ala(94)-mutation contributed significantly to reduced glycogenolysis and less severe hyperglycemia in lipid-exposed humans and was further associated with reduced body weight in a large cohort. Data clearly show that investigation of L-FABP phenotypes in the basal overnight-fasted state yielded incomplete information, and a challenge test was essential to detect phenotypical differences in glucose metabolism between L-FABP genotypes.
肝脏脂肪酸结合蛋白(L-FABP)是脂质代谢中一个高度保守的关键因子。L-FABP中的氨基酸替换可能会改变其功能,从而影响脂质暴露个体的葡萄糖代谢,L-FABP基因敲除小鼠的研究表明了这一点。在1453名白种人队列中对L-FABP中的氨基酸替换进行了研究。在基线时以及320分钟脂质/肝素-生长抑素-胰岛素-胰高血糖素钳夹后,对仅携带常见的苏氨酸(Thr)94位至丙氨酸氨基酸替换(Ala/Ala(94))的健康携带者与年龄、性别和体重指数(BMI)匹配的野生型(Thr/Thr(94))对照者进行了内源性葡萄糖生成(EGP)、糖异生和糖原分解的测量(n = 18)。使用正常血糖-高胰岛素钳夹在无脂质/肝素输注和有脂质/肝素输注的情况下进一步研究了全身葡萄糖处置情况(子集;n = 13)。在整个队列中,唯一常见的Ala/Ala(94)突变与体重减轻显著相关,这与之前的一份报告一致。在脂质暴露、个体匹配的受试者中,EGP存在基因型与脂质治疗的相互作用(P = 0.009),主要是由Ala/Ala(94)携带者中糖原分解减少所驱动(0.46±0.05 vs. 0.59±0.05 mg·kg-1·min-1,P = 0.013)。与野生型相比,Ala/Ala(94)携带者中脂质诱导的血浆葡萄糖水平升高幅度较小(P < 0.0001)。脂质暴露的L-FABP基因型之间的全身葡萄糖处置没有差异。总之,Ala/Ala(94)突变对脂质暴露人群中糖原分解减少和高血糖程度减轻有显著贡献,并且在一个大型队列中还与体重减轻相关。数据清楚地表明,在基础空腹过夜状态下对L-FABP表型的研究产生的信息不完整,挑战试验对于检测L-FABP基因型之间葡萄糖代谢的表型差异至关重要。
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