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胰岛素样生长因子I和生长激素对用 dexamethasone 造成分解代谢的大鼠骨骼肌中泛素系统各组分的调节作用。

Regulation of components of the ubiquitin system by insulin-like growth factor I and growth hormone in skeletal muscle of rats made catabolic with dexamethasone.

作者信息

Chrysis D, Underwood L E

机构信息

Department of Pediatrics, University of North Carolina, Chapel Hill 27599-7220, USA.

出版信息

Endocrinology. 1999 Dec;140(12):5635-41. doi: 10.1210/endo.140.12.7217.

Abstract

To investigate whether the anabolic effects of insulin-like growth factor I (IGF-I) and GH are mediated through regulation of the ubiquitin (Ub) pathway, we examined the effect of IGF-I (0.35 microg/100 g) and/or GH (0.3 mg/100 g BW) on the expression of Ub and Ub-conjugating (E2) enzyme messenger RNAs (mRNAs) in skeletal muscle of rats made catabolic by treatment with dexamethasone (Dex; 0.5 mg/100 g BW) for 3 days. Dex caused a significant loss of body and gastrocnemius weight (14% and 25%, respectively) concurrent with an increase in the 2.8- and 1.2-kb transcripts of Ub (14.3- and 12-fold increases, respectively), the 1.8- and 1.2-kb transcripts of 14-kDa Ub-conjugating enzyme (E2-14 kDa; 5.6- and 7.7-fold increases, respectively), the 4.4- and 2.4-kb transcripts of Ub-E2G (6.5- and 8.2-fold increases, respectively), and the 2E isoform of the 17-kDa E2 mRNA (3.5-fold increase). Injections of IGF-I in Dex-treated animals ameliorated the body weight loss, and the gastrocnemius tended to be heavier. This improvement was also accompanied by a significant suppression of transcripts for Ub (58% and 66% decreases), E2-14 kDa (58% and 68% decreases), and Ub-E2G (78% decrease), whereas the 2E isoform of the 17-kDa E2 was only modestly affected (20% decrease). GH restored serum IGF-I levels to normal in Dex-treated rats, but had no effect on the body weight loss or on any of the studied components of the Ub pathway. Administration of IGF-I to the Dex/GH-treated animals decreased the activated mRNAs of the Ub pathway in a manner and degree similar to those observed in the Dex/ IGF-I group. In summary, these results provide evidence that IGF-I regulates the expression of mRNAs encoding components of the Ub pathway during catabolism and suggest a possible mechanism for the antiproteolytic actions of IGF-I. On the other hand, GH, which is believed not to affect proteolysis but only protein synthesis, had no effect on any of the mRNAs studied.

摘要

为了研究胰岛素样生长因子I(IGF-I)和生长激素(GH)的合成代谢作用是否通过泛素(Ub)途径的调节介导,我们检测了IGF-I(0.35微克/100克)和/或GH(0.3毫克/100克体重)对用0.5毫克/100克体重的地塞米松(Dex)处理3天而导致分解代谢的大鼠骨骼肌中Ub和Ub结合(E2)酶信使核糖核酸(mRNA)表达的影响。Dex导致体重和腓肠肌重量显著下降(分别为14%和25%),同时Ub的2.8和1.2千碱基转录本增加(分别增加14.3倍和12倍),14千道尔顿Ub结合酶(E2-14 kDa)的1.8和1.2千碱基转录本增加(分别增加5.6倍和7.7倍),Ub-E2G的4.4和2.4千碱基转录本增加(分别增加6.5倍和8.2倍),以及17千道尔顿E2 mRNA的2E异构体增加(增加3.5倍)。给Dex处理的动物注射IGF-I改善了体重减轻,腓肠肌也趋于更重。这种改善还伴随着Ub转录本(分别下降58%和66%)、E2-14 kDa(分别下降58%和68%)和Ub-E2G(下降78%)的显著抑制,而17千道尔顿E2的2E异构体仅受到轻微影响(下降20%)。GH使Dex处理的大鼠血清IGF-I水平恢复正常,但对体重减轻或Ub途径的任何研究成分均无影响。给Dex/GH处理的动物施用IGF-I,以与Dex/IGF-I组中观察到的方式和程度相似的方式降低了Ub途径的活化mRNA。总之,这些结果提供了证据表明IGF-I在分解代谢过程中调节编码Ub途径成分的mRNA的表达,并提示了IGF-I抗蛋白水解作用的可能机制。另一方面,据信不影响蛋白水解而仅影响蛋白质合成的GH,对任何研究的mRNA均无影响。

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