首页> 外文期刊>American Journal of Physiology >Effect of pulsatile growth hormone administration to the growth-restricted fetal sheep on somatotrophic axis gene expression in fetal and placental tissues.
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Effect of pulsatile growth hormone administration to the growth-restricted fetal sheep on somatotrophic axis gene expression in fetal and placental tissues.

机译:向生长受限的绵羊施用搏动性生长激素对胎儿和胎盘组织中营养轴基因表达的影响。

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摘要

We have previously reported (Bauer MK, Breier BH, Bloomfield FH, Jensen EC, Gluckman PD, and Harding JE. J Endocrinol 177: 83-92, 2003) that a chronic pulsatile infusion of growth hormone (GH) to intrauterine growth-restricted (IUGR) ovine fetuses increased fetal circulating IGF-I levels without increasing fetal growth. We hypothesized a cortisol-induced upregulation of fetal hepatic GH receptor (GH-R) mRNA levels, secondary increases in IGF-I mRNA levels, and circulating IGF-I levels, but a downregulation of the type I IGF receptor (IGF-IR) as an explanation. We, therefore, measured mRNA levels of genes of the somatotrophic axis by real-time RT-PCR in fetal and placental tissues of fetuses with IUGR (induced by uteroplacental embolization from 110- to 116-days gestation) that received either a pulsatile infusion of GH (total dose 3.5 mg/day) or vehicle from 117-126 days and in control fetuses (n = 5 per group). Tissues were collected at 127 days (term, 145 days). Fetal cortisol concentrations were significantly increased in IUGR fetuses. However, in liver, GH-R, but not IGF-I or IGF-IR, mRNA levels were decreased in both IUGR groups. In contrast, in placenta, GH-R, IGF-I, and IGF-IR expression were increased in IUGR vehicle-infused fetuses. GH infusion further increased placental GH-R and IGF-IR, but abolished the increase in IGF-I mRNA levels. GH infusion reduced IGF-I expression in muscle and increased GH-R but decreased IGF-IR expression in kidney. IUGR increased hepatic IGF-binding protein (IGFBP)-1 and placental IGFBP-2 and -3 mRNA levels with no further effect of GH infusion. In conclusion, the modest increases in circulating cortisol concentrations in IUGR fetuses did not increase hepatic GH-R mRNA expression and, therefore, do not explain the increased circulating IGF-I levels that we found with GH infusion, which are likely due to reduced clearance rather than increased production. We demonstrate tissue-specific regulation of the somatotrophic axis in IUGR fetuses and a discontinuity between GH-R and IGF-I gene expression in GH-infused fetuses that is not explained by alterations in phosphorylated STAT5b.
机译:我们以前曾报道过(鲍尔·M·K,布雷尔·BH,布卢姆菲尔德·FH,詹森·EC,格鲁克曼PD和哈丁·J·J·内分泌177:83-92,2003年),长期以脉冲方式注入生长激素(GH)限制了子宫内的生长。 (IUGR)绵羊胎儿在不增加胎儿生长的情况下增加了胎儿循环IGF-I水平。我们假设皮质醇诱导胎儿肝GH受体(GH-R)mRNA水平上调,IGF-I mRNA水平继发性增加和循环IGF-1水平,但I型IGF受体(IGF-IR)下调作为解释。因此,我们通过实时RT-PCR测定了IUGR胎儿(在妊娠110-116天时由子宫胎盘栓塞诱导)的胎儿和胎盘组织中营养轴基因的mRNA水平,该脉冲或输注是GH(总剂量3.5 mg /天)或赋形剂在117-126天及对照组胎儿中(每组n = 5)。在127天(足月145天)收集组织。 IUGR胎儿的胎儿皮质醇浓度显着增加。然而,在肝脏中,GHR-而不是IGF-1或IGF-1R在两个IUGR组中均降低了mRNA水平。相反,在注入IUGR媒介物的胎儿中,胎盘中的GH-R,IGF-I和IGF-IR表达增加。 GH注入进一步增加了胎盘GH-R和IGF-IR,但取消了IGF-I mRNA水平的增加。 GH注入可降低肌肉中IGF-I的表达,并增加GH-R,但可降低肾脏中IGF-IR的表达。 IUGR增加了肝IGF结合蛋白(IGFBP)-1和胎盘IGFBP-2和-3 mRNA的水平,而GH的注入没有进一步的影响。总之,IUGR胎儿中循环皮质醇浓度的适度增加不会增加肝脏GH-R mRNA表达,因此,不能解释我们在GH输注时发现的循环IGF-I水平升高,这很可能是由于清除率降低所致而不是增加产量。我们证明了IUGR胎儿的营养轴的组织特异性调节以及GH注入的胎儿中GH-R和IGF-I基因表达之间的不连续性,这不能通过磷酸化STAT5b的改变来解释。

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