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对接受胰岛素样生长因子(IGF)-I或生长激素治疗的胃肠外营养大鼠空肠中胰岛素样生长因子(IGF)-I与胰岛素受体结合及表达的研究。

Investigation of insulin-like growth factor (IGF)-I and insulin receptor binding and expression in jejunum of parenterally fed rats treated with IGF-I or growth hormone.

作者信息

Ney D M, Huss D J, Gillingham M B, Kritsch K R, Dahly E M, Talamantez J L, Adamo M L

机构信息

Department of Nutritional Sciences, University of Wisconsin-Madison, 53706, USA.

出版信息

Endocrinology. 1999 Oct;140(10):4850-60. doi: 10.1210/endo.140.10.7029.

DOI:10.1210/endo.140.10.7029
PMID:10499545
Abstract

To investigate the ability of insulin-like growth factor-I (IGF-I), but not GH, to stimulate jejunal growth, we compared indices of IGF-I and insulin receptor expression in jejunal membranes from rats maintained with total parenteral nutrition (TPN) and treated with rhIGF-I and/or rhGH. TPN without growth factor treatment (TPN control) induced jejunal atrophy, reduced serum IGF-I, increased serum insulin concentrations, and increased IGF-I receptor number, IGF-I receptor messenger RNA, and insulin-specific binding to 133% to 170% of the orally fed reference values, P < 0.01. Compared with TPN control, IGF-I or IGF-I + GH stimulated jejunal mucosal hyperplasia; IGF-I treatment increased serum IGF-I by 2- to 3-fold and decreased serum insulin concentrations by 60%, decreased IGF-I receptor number by 50% (P < 0.001), and increased insulin receptor affinity and insulin receptor protein content. Treatment with GH alone increased serum IGF-I concentration, did not alter TPN-induced jejunal atrophy, and decreased insulin-specific binding and insulin receptor protein content (39% and 59%, respectively, of the TPN control values, P < 0.01). We conclude that: 1) jejunal IGF-I receptor content reflects circulating concentration of ligand and is not limiting for jejunal growth; and 2) increased circulating concentration of IGF-I may promote jejunal growth via interaction with jejunal insulin or IGF-I receptors.

摘要

为了研究胰岛素样生长因子-I(IGF-I)而非生长激素(GH)刺激空肠生长的能力,我们比较了接受全胃肠外营养(TPN)并接受重组人IGF-I和/或重组人生长激素治疗的大鼠空肠膜中IGF-I和胰岛素受体表达指标。未进行生长因子治疗的TPN(TPN对照组)导致空肠萎缩,血清IGF-I降低,血清胰岛素浓度升高,IGF-I受体数量、IGF-I受体信使核糖核酸增加,胰岛素特异性结合增加至经口喂养参考值的133%至170%,P<0.01。与TPN对照组相比,IGF-I或IGF-I+GH刺激空肠黏膜增生;IGF-I治疗使血清IGF-I升高2至3倍,血清胰岛素浓度降低60%,IGF-I受体数量减少50%(P<0.001),并增加胰岛素受体亲和力和胰岛素受体蛋白含量。单独使用GH治疗可提高血清IGF-I浓度,不改变TPN诱导的空肠萎缩,并降低胰岛素特异性结合和胰岛素受体蛋白含量(分别为TPN对照组值的39%和59%,P<0.01)。我们得出结论:1)空肠IGF-I受体含量反映配体的循环浓度,对空肠生长无限制作用;2)循环中IGF-I浓度升高可能通过与空肠胰岛素或IGF-I受体相互作用促进空肠生长。

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