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克伦特罗可诱导大鼠背阔肌和心脏肥大,并伴有分子和表型变化。

Clenbuterol induces hypertrophy of the latissimus dorsi muscle and heart in the rat with molecular and phenotypic changes.

作者信息

Petrou M, Wynne D G, Boheler K R, Yacoub M H

机构信息

Royal Brompton National Heart and Lung Institute, London, UK.

出版信息

Circulation. 1995 Nov 1;92(9 Suppl):II483-9. doi: 10.1161/01.cir.92.9.483.

Abstract

BACKGROUND

Skeletal muscle assistance of the circulation for patients in end-stage heart failure requires electrical training of the latissimus dorsi flap to produce fatigue resistance. This process of electrical transformation and the development of postmobilization atrophy results in a profound loss in peak power generated. The beta 2-adrenoceptor agonist clenbuterol was used to investigate its potential to selectively induce skeletal muscle hypertrophy, particularly the latissimus dorsi muscle (LDM), independent of adverse effects on cardiac muscle.

METHODS AND RESULTS

Forty-one male Sprague-Dawley rats were divided into four groups and used in this study. Clenbuterol 2 micrograms.g body wt-1.d-1 was administered subcutaneously for a period of either 5 weeks (group A) or 2 weeks (group A1). Groups B and B1 (controls) were injected with 0.5 mL normal saline once daily. At the end of the experimental period, all rats were weighed and terminally anesthetized for removal of the left LDM, left gastrocnemius-plantaris-soleus (GPS) muscles, and heart. The results showed that the increase in body weight did not differ significantly between the clenbuterol-treated and control groups (P > .5). The ratio of LDM to tibial length (hypertrophic index) for groups A and A1 was significantly greater than controls (P < .01), which represented a 20% to 29% increase. The hypertrophy was more pronounced for hindlimb skeletal muscle (21% to 35% for GPS), and the effects of this relatively high dose of clenbuterol on the heart were less marked (18% to 20% hypertrophy). RNA analyses indicate that ventricles of clenbuterol-treated rats express elevated levels of mRNA to atrial natriuretic factor without a concomitant increase in skeletal alpha-actin and beta-myosin heavy chain, consistent with a "physiological" form of cardiac hypertrophy.

CONCLUSIONS

Clenbuterol induces significant hypertrophy of the LDM associated with specific changes in cardiac gene expression.

摘要

背景

对于终末期心力衰竭患者,骨骼肌辅助循环需要对背阔肌皮瓣进行电刺激训练以产生抗疲劳能力。这种电刺激转化过程以及运动后萎缩的发展会导致产生的峰值功率大幅下降。使用β2 -肾上腺素能受体激动剂克仑特罗来研究其选择性诱导骨骼肌肥大的潜力,特别是背阔肌(LDM),同时避免对心肌产生不良影响。

方法与结果

41只雄性Sprague - Dawley大鼠被分为四组用于本研究。克仑特罗以2微克·克体重-1·天-1的剂量皮下给药,持续5周(A组)或2周(A1组)。B组和B1组(对照组)每天注射0.5毫升生理盐水。实验期末,对所有大鼠称重并进行终末麻醉,以切除左侧背阔肌、左侧腓肠肌 - 比目鱼肌(GPS)和心脏。结果显示,克仑特罗治疗组与对照组之间体重增加无显著差异(P > 0.5)。A组和A1组背阔肌与胫骨长度的比值(肥大指数)显著高于对照组(P < 0.01),增幅为20%至29%。后肢骨骼肌的肥大更为明显(GPS为21%至35%),而这种相对高剂量的克仑特罗对心脏的影响较小(肥大18%至20%)。RNA分析表明,克仑特罗治疗大鼠的心室中,心房利钠肽的mRNA表达水平升高,而骨骼肌α -肌动蛋白和β -肌球蛋白重链没有相应增加,这与心脏肥大的“生理性”形式一致。

结论

克仑特罗可诱导背阔肌显著肥大,并伴有心脏基因表达的特定变化。

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