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孕期热量限制小鼠体内的胃饥饿素、胃饥饿素O-酰基转移酶与碳水化合物代谢

Ghrelin, Ghrelin O-Acyltransferase, and Carbohydrate Metabolism During Pregnancy in Calorie-Restricted Mice.

作者信息

Trivedi Arjun, Babic Sandra, Heiman Mark, Gibson William T, Chanoine Jean-Pierre

机构信息

Child & Family Research Institute, Vancouver, BC, Canada.

MicroBiome Therapeutics, New Orleans, LA, USA.

出版信息

Horm Metab Res. 2017 Jan;49(1):64-72. doi: 10.1055/s-0042-116117. Epub 2016 Oct 4.

Abstract

Acylation of ghrelin is mediated by ghrelin acyltansferase (GOAT). Exogenous acylated ghrelin (AG) stimulates growth hormone (GH) and food intake. In non-pregnant (NP) animals, the GOAT-ghrelin-GH axis prevents hypoglycemia caused by caloric restriction (CR). In humans, maternal malnutrition challenges glucose metabolism, which is a key determinant of fetal health. To clarify the role of AG and GH, we compared effects of CR on the GOAT-ghrelin-GH axis in pregnant (P) and NP mice. C57BL/6 wild type (WT) and GOAT knock-out (KO) P and NP mice were freely fed (FF) or subjected to 50% CR for one week. CR was started in P mice on Day 10.5 after conception. We measured body composition, blood glucose, plasma ghrelin and GH, stomach, hypothalamus and pituitary GOAT and ghrelin expression, and liver glycogen content and expression. GOAT and AG were undetectable in KO. In NP mice, CR did not affect blood glucose (-1.3 mmol/l, p>0.05) in WT but was lowered (-1.8 mmol/l, p<0.0001) in KO. GH and mRNA expression increased in WT but not in KO. In P mice, CR markedly lowered glucose (-2.7 mmol/l; p<0.0001) in WT and caused fatal hypoglycemia in KO, despite similarly elevated GH in WT and KO mice. KO animals are more prone to hypoglycemia than WT. GH, which is high in P animals, does not prevent hypoglycemia caused by CR during pregnancy. Our data suggest a specific role of AG in the regulation of gluconeogenesis to maintain euglycemia during pregnancy when energy availability is limited.

摘要

胃饥饿素的酰化作用由胃饥饿素酰基转移酶(GOAT)介导。外源性酰化胃饥饿素(AG)可刺激生长激素(GH)分泌并促进食物摄入。在非妊娠(NP)动物中,GOAT-胃饥饿素-GH轴可预防因热量限制(CR)导致的低血糖。在人类中,母体营养不良会影响葡萄糖代谢,而葡萄糖代谢是胎儿健康的关键决定因素。为了阐明AG和GH的作用,我们比较了CR对妊娠(P)和NP小鼠GOAT-胃饥饿素-GH轴的影响。将C57BL/6野生型(WT)和GOAT基因敲除(KO)的P和NP小鼠分为自由进食(FF)组或进行为期一周的50%CR处理组。P小鼠在受孕后第10.5天开始进行CR处理。我们测量了身体组成、血糖、血浆胃饥饿素和GH水平,胃、下丘脑和垂体中GOAT和胃饥饿素的表达,以及肝脏糖原含量和表达。在KO小鼠中未检测到GOAT和AG。在NP小鼠中,CR对WT小鼠的血糖没有影响(-1.3 mmol/l,p>0.05),但在KO小鼠中血糖降低(-1.8 mmol/l,p<0.0001)。WT小鼠中GH和mRNA表达增加,而KO小鼠中未增加。在P小鼠中,CR使WT小鼠的血糖显著降低(-2.7 mmol/l;p<0.0001),并导致KO小鼠出现致命性低血糖,尽管WT和KO小鼠中的GH升高程度相似。KO动物比WT动物更容易发生低血糖。P动物中较高的GH水平并不能预防妊娠期间CR导致的低血糖。我们的数据表明,在能量供应有限的妊娠期,AG在调节糖异生以维持血糖正常方面具有特定作用。

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