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生长激素(GH)对大鼠肝脏中胰岛素样生长因子I和GH受体/结合蛋白基因表达的差异调节

Differential regulation by growth hormone (GH) of insulin-like growth factor I and GH receptor/binding protein gene expression in rat liver.

作者信息

Maiter D, Walker J L, Adam E, Moatsstaats B, Mulumba N, Ketelslegers J M, Underwood L E

机构信息

Unité de Diabétologie et Nutrition, University of Louvain School of Medicine, Brussels, Belgium.

出版信息

Endocrinology. 1992 Jun;130(6):3257-64. doi: 10.1210/endo.130.6.1375898.

Abstract

We have reported that female hypophysectomized (hypox) rats replaced with T4 and cortisone and treated for 7 days with GH injections (4 x 12.5 micrograms/day) had significantly greater growth and increase in serum insulin-like growth factor-I (IGF-I) than did hypox rats continuously infused with GH (50 and 250 micrograms/day), whereas GH binding to liver membranes was increased only by infusion. We now report the effects of hypophysectomy, T4 and cortisone replacement, and the aforementioned continuous vs. intermittent GH treatment on liver IGF-I and GH receptor (GHR)/binding protein (GHBP) gene expression in female rats. Concentrations of IGF-I peptide were measured in acid-extracted sera and liver tissues. Total GH binding to liver membranes was determined in MgCl2-treated homogenates and serum GH binding activity was assessed by gel filtration of serum incubated with 125I-bovine GH. The abundance of messenger RNA (mRNA) transcripts encoding IGF-I, the GHR, and the GHBP was quantified by Northern hybridization analysis of liver poly(A)+ RNA. Hypophysectomy in female animals decreased serum IGF-I and liver IGF-I mRNA concentrations by 95% and 87%, respectively, serum GHBP activity, and total liver GH binding by 50% (P less than 0.001 compared with intact controls), and liver GHR and GHBP mRNA abundance by 30-35% (P less than 0.05 vs. controls). These changes were not reversed by T4 and cortisone treatment. Repeated injections of GH produced a 13-fold increase in liver IGF-I peptide and a 5-fold increase in liver IGF-I mRNA concentrations (vs. saline-treated hypox rats), whereas continuous GH infusions induced only 7-fold and 2-fold increases in IGF-I peptide and mRNA, respectively. Serum GHBP activity was not changed in the GH-injected animals, but rose 2- to 3-fold in the GH-infused rats, an increase similar to that reported for their liver GH binding sites. No major change in liver concentrations of GHR and GHBP mRNAs was seen after repeated GH injections. Differential regulation of the two GHR/GHBP gene products was observed after continuous infusion of GH, with a net 60-70% increase in liver GHBP mRNA abundance contrasting with no apparent change in the GHR mRNA transcript. These results indicate that pulsatile GH administration is more effective than continuous GH infusion in stimulating liver IGF-I gene expression, and this effect is not mediated by an increase in GHR mRNA or protein.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

我们曾报道,雌性垂体切除(hypox)大鼠补充T4和可的松,并每日注射生长激素(GH)(4×12.5微克/天),连续治疗7天,其生长显著加快,血清胰岛素样生长因子-I(IGF-I)增加幅度显著大于持续输注GH(50和250微克/天)的hypox大鼠,而只有输注GH才能增加肝脏膜上的GH结合。我们现在报告垂体切除、T4和可的松补充以及上述持续与间歇GH治疗对雌性大鼠肝脏IGF-I和GH受体(GHR)/结合蛋白(GHBP)基因表达的影响。在酸提取的血清和肝脏组织中测量IGF-I肽的浓度。在MgCl2处理的匀浆中测定肝脏膜上总的GH结合,并通过对与125I-牛GH孵育的血清进行凝胶过滤来评估血清GH结合活性。通过对肝脏多聚腺苷酸(poly(A)+)RNA进行Northern杂交分析,定量编码IGF-I、GHR和GHBP的信使RNA(mRNA)转录本的丰度。雌性动物垂体切除后,血清IGF-I和肝脏IGF-I mRNA浓度分别降低95%和87%,血清GHBP活性以及肝脏总的GH结合降低50%(与完整对照相比,P<0.001),肝脏GHR和GHBP mRNA丰度降低30 - 35%(与对照相比,P<0.05)。T4和可的松治疗未能逆转这些变化。重复注射GH使肝脏IGF-I肽增加13倍,肝脏IGF-I mRNA浓度增加5倍(与盐水处理的hypox大鼠相比),而持续输注GH分别仅使IGF-I肽和mRNA增加7倍和2倍。注射GH的动物血清GHBP活性未改变,但在输注GH的大鼠中升高2至3倍,这一增加与报道的其肝脏GH结合位点的增加相似。重复注射GH后,肝脏GHR和GHBP mRNA浓度未见重大变化。持续输注GH后观察到两种GHR/GHBP基因产物的差异调节,肝脏GHBP mRNA丰度净增加60 - 70%,而GHR mRNA转录本无明显变化。这些结果表明,脉冲式给予GH在刺激肝脏IGF-I基因表达方面比持续输注GH更有效,且这种作用不是由GHR mRNA或蛋白增加介导的。(摘要截短至400字)

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