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妊娠早期母体内分泌胰岛素样生长因子I可使胎盘在整个妊娠期具备更强的功能能力。

Early pregnancy maternal endocrine insulin-like growth factor I programs the placenta for increased functional capacity throughout gestation.

作者信息

Sferruzzi-Perri Amanda N, Owens Julie A, Standen Prue, Taylor Robyn L, Robinson Jeffrey S, Roberts Claire T

机构信息

Research Centre for Reproductive Health, Discipline of Obstetrics and Gynaecology, School of Paediatrics and Reproductive Health, University of Adelaide, Adelaide, South Australia 5005, Australia.

出版信息

Endocrinology. 2007 Sep;148(9):4362-70. doi: 10.1210/en.2007-0411. Epub 2007 May 24.

Abstract

In early pregnancy, the concentrations of IGFs increase in maternal blood. Treatment of pregnant guinea pigs with IGFs in early to midpregnancy enhances placental glucose transport and fetal growth and viability near term. In the current study, we determined whether exogenous IGFs altered placental gene expression, transport, and nutrient partitioning during treatment, which may then persist. Guinea pigs were infused with IGF-I, IGF-II (both 1 mg/kg x d) or vehicle sc from d 20-35 of pregnancy and killed on d 35 (term is 70 d) after administration of [(3)H]methyl-D-glucose (MG) and [(14)C]amino-isobutyric acid (AIB). IGF-I increased placental and fetal weights (+15 and +17%, respectively) and MG and AIB uptake by the placenta (+42 and +68%, respectively) and fetus (+59 and +90%, respectively). IGF-I increased placental mRNA expression of the amino acid transporter gene Slc38a2 (+780%) and reduced that of Igf2 (-51%), without altering the glucose transporter Slc2a1 or Vegf and Igf1 genes. There were modest effects of IGF-I treatment on MG and AIB uptake by individual maternal tissues and no effect on plasma glucose, total amino acids, free fatty acids, triglycerides, and cholesterol concentrations. IGF-II treatment of the mother did not alter any maternal, fetal or placental parameter. In conclusion, exogenous IGF-I, but not IGF-II, in early pregnancy increases placental transport of MG and AIB, enhancing midgestational fetal nutrient uptake and growth. This suggests that early pregnancy rises in maternal circulating IGF-I play a major role in regulating placental growth and functional development and thus fetal growth throughout gestation.

摘要

在妊娠早期,母体血液中胰岛素样生长因子(IGFs)的浓度会升高。在妊娠早期至中期用IGFs治疗怀孕的豚鼠,可增强胎盘葡萄糖转运以及接近足月时胎儿的生长和活力。在本研究中,我们确定了外源性IGFs在治疗期间是否会改变胎盘基因表达、转运和营养分配,而这些改变可能会持续存在。从妊娠第20天至35天,给豚鼠皮下注射IGF-I、IGF-II(均为1 mg/kg×d)或赋形剂,在给予[³H]甲基-D-葡萄糖(MG)和[¹⁴C]氨基异丁酸(AIB)后,于第35天(足月为70天)处死豚鼠。IGF-I增加了胎盘和胎儿的重量(分别增加15%和17%),胎盘对MG和AIB的摄取量(分别增加42%和68%)以及胎儿对MG和AIB的摄取量(分别增加59%和90%)。IGF-I增加了氨基酸转运蛋白基因Slc38a2的胎盘mRNA表达(增加780%),并降低了Igf2的表达(降低51%),而未改变葡萄糖转运蛋白Slc2a1或Vegf和Igf1基因的表达。IGF-I治疗对母体各组织对MG和AIB的摄取有适度影响,对血浆葡萄糖、总氨基酸、游离脂肪酸、甘油三酯和胆固醇浓度无影响。对母体进行IGF-II治疗未改变任何母体、胎儿或胎盘参数。总之,妊娠早期外源性IGF-I而非IGF-II可增加胎盘对MG和AIB的转运,增强妊娠中期胎儿的营养摄取和生长。这表明母体循环中IGF-I在妊娠早期的升高在调节胎盘生长和功能发育以及整个妊娠期胎儿生长中起主要作用。

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