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生长激素在体内刺激c-myc和胰岛素样生长因子I表达的顺序诱导。

Growth hormone stimulates sequential induction of c-myc and insulin-like growth factor I expression in vivo.

作者信息

Murphy L J, Bell G I, Friesen H G

出版信息

Endocrinology. 1987 May;120(5):1806-12. doi: 10.1210/endo-120-5-1806.

Abstract

The effect of GH administration to hypophysectomized rats on expression of the c-myc proto-oncogene and insulin-like growth factor I (IGF-I) in the liver and kidney was examined. In both tissues maximal expression of c-myc occurred by 1 h after a single injection of human GH (100 micrograms/100 g bw). In the liver the maximal c-myc mRNA level was increased 12 +/- 3.9-fold (mean +/- SEM; n = 4), while the maximal c-myc level in the kidney was increased 3.4-fold (n = 2) compared to levels in basal hypophysectomized rats. In both the liver and kidney the IGF-I cDNA hybridized under stringent conditions to three transcripts with apparent sizes of 7.0, 1.8, and diffuse group of transcripts of 0.7-1.1 kilobases. Each of these transcripts demonstrated some degree of GH dependence. Under the hybridization condition used, the 7.0-kilobase IGF-I mRNA was virtually undetectable in the hypophysectomized control rat liver, while the smaller transcripts were easily detectable. Peak expression of each of the IGF-I transcripts occurred 6-12 h after GH administration. Maximal IGF-I expression in the kidney occurred 9 h after the GH injection. To determine whether the increase in c-myc expression following GH could result from a small but undetectable increase in IGF-I expression in these tissues, we administered human recombinant IGF-I to hypophysectomized rats (50 micrograms/100 g bw, ip). Despite a significant increase in serum IGF-I concentrations to levels greater than those present in the first 3 h after GH administration, no increase in c-myc expression was apparent in either the liver or kidney. These observations suggest that GH itself, rather than IGF-I, initiates the mitogenic response in the liver and kidney that follows GH administration to hypophysectomized rats.

摘要

研究了给垂体切除大鼠注射生长激素(GH)对肝脏和肾脏中c-myc原癌基因及胰岛素样生长因子I(IGF-I)表达的影响。在这两种组织中,单次注射人GH(100微克/100克体重)后1小时,c-myc出现最大表达。与垂体切除的基础大鼠相比,肝脏中c-myc mRNA的最大水平增加了12±3.9倍(平均值±标准误;n = 4),而肾脏中c-myc的最大水平增加了3.4倍(n = 2)。在肝脏和肾脏中,IGF-I cDNA在严格条件下与三种转录本杂交,其表观大小分别为7.0、1.8以及0.7 - 1.1千碱基的弥散转录本组。这些转录本均表现出一定程度的GH依赖性。在所使用的杂交条件下,垂体切除的对照大鼠肝脏中几乎检测不到7.0千碱基的IGF-I mRNA,而较小的转录本则易于检测到。每种IGF-I转录本的峰值表达在GH给药后6 - 12小时出现。肾脏中IGF-I的最大表达在GH注射后9小时出现。为了确定GH后c-myc表达的增加是否可能源于这些组织中IGF-I表达的微小但不可检测的增加,我们给垂体切除的大鼠腹腔注射人重组IGF-I(50微克/100克体重)。尽管血清IGF-I浓度显著增加至高于GH给药后最初3小时的水平,但肝脏或肾脏中c-myc表达均未明显增加。这些观察结果表明,在给垂体切除大鼠注射GH后,是GH本身而非IGF-I引发了肝脏和肾脏中的促有丝分裂反应。

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