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正常小鼠和营养不良小鼠中肌源性调节因子的表达:胰岛素样生长因子-1治疗的影响

Expression of myogenic regulatory factors in normal and dystrophic mice: effects of IGF-1 treatment.

作者信息

Hsu H H, Zdanowicz M M, Agarwal V R, Speiser P W

机构信息

Department of Pediatrics, North Shore University Hospital-New York University School of Medicine, Manhasset 11030, USA.

出版信息

Biochem Mol Med. 1997 Apr;60(2):142-8. doi: 10.1006/bmme.1997.2570.

Abstract

Myogenic regulatory factors (MRFs) promote differentiation of muscle cells from fibroblasts and are induced by insulin-like growth factor I (IGF-1). Prior studies have shown synthesis of new muscle protein and improved muscle morphology when mature dy mice with muscular dystrophy are treated with IGF-1. We investigated whether these salutary effects of IGF-1 might be attributable to stimulation of MRFs. Male dy (129ReJ) mice and controls (129J) were assigned to IGF-1 treatment (10 micrograms twice daily) or non-treatment at about 5 weeks of life and sacrificed 6 weeks later. RNA was extracted from skeletal muscles, reverse transcribed, and amplified by polymerase chain reaction (PCR) using primers specific for each MRF. Competitive PCR was performed to quantify MyoD expression in response to IGF-1 treatment. Transcripts for myf-5, MRF4, and myogenin were detected in both control and dy mouse muscles; no apparent differences were observed between treatment groups. Quantitative analysis of transcripts for MyoD indicated no significant basal differences between control and dy mice. There was, however, significantly higher MyoD expression in the dy group, and a trend toward significance in the control group, following IGF-1 treatment. These data suggest that IGF-1 exerts its in vivo effects in postembryonal muscle by stimulating MRFs.

摘要

生肌调节因子(MRFs)促进成纤维细胞向肌肉细胞分化,并由胰岛素样生长因子I(IGF-1)诱导产生。先前的研究表明,用IGF-1治疗患有肌肉萎缩症的成年dy小鼠时,会合成新的肌肉蛋白并改善肌肉形态。我们研究了IGF-1的这些有益作用是否可能归因于对MRFs的刺激。将雄性dy(129ReJ)小鼠和对照组(129J)在大约5周龄时分为IGF-1治疗组(每日两次,每次10微克)或非治疗组,6周后处死。从骨骼肌中提取RNA,进行逆转录,并使用针对每个MRF的特异性引物通过聚合酶链反应(PCR)进行扩增。进行竞争性PCR以定量响应IGF-1治疗的MyoD表达。在对照和dy小鼠肌肉中均检测到myf-5、MRF4和肌细胞生成素的转录本;治疗组之间未观察到明显差异。对MyoD转录本的定量分析表明,对照和dy小鼠之间的基础水平无显著差异。然而,在IGF-1治疗后,dy组中MyoD的表达显著更高,对照组有显著趋势。这些数据表明,IGF-1通过刺激MRFs在胚胎后肌肉中发挥其体内作用。

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