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搏动性高血糖会增加宫内生长受限胎儿绵羊的胰岛素分泌,但不会增加胰腺β细胞质量。

Pulsatile hyperglycemia increases insulin secretion but not pancreatic β-cell mass in intrauterine growth-restricted fetal sheep.

作者信息

Boehmer B H, Brown L D, Wesolowski S R, Hay W W, Rozance P J

机构信息

Department of Pediatrics,Perinatal Research Center,University of Colorado School of Medicine,Aurora,CO,USA.

出版信息

J Dev Orig Health Dis. 2018 Oct;9(5):492-499. doi: 10.1017/S2040174418000417. Epub 2018 Jul 5.

Abstract

Impaired β-cell development and insulin secretion are characteristic of intrauterine growth-restricted (IUGR) fetuses. In normally grown late gestation fetal sheep pancreatic β-cell numbers and insulin secretion are increased by 7-10 days of pulsatile hyperglycemia (PHG). Our objective was to determine if IUGR fetal sheep β-cell numbers and insulin secretion could also be increased by PHG or if IUGR fetal β-cells do not have the capacity to respond to PHG. Following chronic placental insufficiency producing IUGR in twin gestation pregnancies (n=7), fetuses were administered a PHG infusion, consisting of 60 min, high rate, pulsed infusions of dextrose three times a day with an additional continuous, low-rate infusion of dextrose to prevent a decrease in glucose concentrations between the pulses or a control saline infusion. PHG fetuses were compared with their twin IUGR fetus, which received a saline infusion for 7 days. The pulsed glucose infusion increased fetal arterial glucose concentrations an average of 83% during the infusion. Following the 7-day infusion, a square-wave fetal hyperglycemic clamp was performed in both groups to measure insulin secretion. The rate of increase in fetal insulin concentrations during the first 20 min of a square-wave hyperglycemic clamp was 44% faster in the PHG fetuses compared with saline fetuses (P0.23). Chronic PHG increases early phase insulin secretion in response to acute hyperglycemia, indicating that IUGR fetal β-cells are functionally responsive to chronic PHG.

摘要

β细胞发育受损和胰岛素分泌异常是宫内生长受限(IUGR)胎儿的特征。在正常生长的妊娠晚期绵羊胎儿中,7 - 10天的脉冲式高血糖(PHG)可增加胰腺β细胞数量和胰岛素分泌。我们的目的是确定PHG是否也能增加IUGR胎儿绵羊的β细胞数量和胰岛素分泌,或者IUGR胎儿β细胞是否没有能力对PHG作出反应。在双胎妊娠中通过慢性胎盘功能不全导致IUGR(n = 7)后,给胎儿进行PHG输注,包括每天三次60分钟的高频率葡萄糖脉冲输注,以及额外的持续低速率葡萄糖输注以防止脉冲之间葡萄糖浓度下降,或进行对照生理盐水输注。将接受PHG输注的胎儿与其接受7天生理盐水输注的双胎IUGR胎儿进行比较。脉冲式葡萄糖输注期间胎儿动脉葡萄糖浓度平均增加83%。7天输注后,两组均进行方波胎儿高血糖钳夹以测量胰岛素分泌。与生理盐水组胎儿相比,PHG组胎儿在方波高血糖钳夹的前20分钟内胎儿胰岛素浓度的增加速率快44%(P0.23)。慢性PHG可增加对急性高血糖的早期胰岛素分泌,表明IUGR胎儿β细胞对慢性PHG有功能反应。

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Chronic anemic hypoxemia attenuates glucose-stimulated insulin secretion in fetal sheep.慢性贫血性低氧血症会减弱胎羊的葡萄糖刺激的胰岛素分泌。
Am J Physiol Regul Integr Comp Physiol. 2017 Apr 1;312(4):R492-R500. doi: 10.1152/ajpregu.00484.2016. Epub 2017 Jan 18.

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