1‐Sarcosine–angiotensin II infusion effects on food intake, weight loss, energy expenditure, and skeletal muscle UCP3 gene expression in a rat model

Cichello S. A.; Schuijers J.; Weisinger R. S.

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1‐Sarcosine–angiotensin II infusion effects on food intake, weight loss, energy expenditure, and skeletal muscle UCP3 gene expression in a rat model

机译：1-Sarcosine-Angiotensin II输注对大鼠模型中食物摄入，体重减轻，能量消耗和骨骼肌UCP3基因表达的影响

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AbstractBackgroundThere are a myriad of proteins responsible for modulation of expenditure of energy. Angiotensin II (Ang II) is a vital component of renin-angiotensin system that affects blood pressure and also linked to both cachexia and obesity via fat and muscle metabolism. Previous research suggests that the direct action of Ang II is on the brain, via angiotensin II type 1 receptor protein, affecting food intake and energy expenditure. The objective of the study is to investigate the effect of 1-sarcosine (SAR)-Ang II infusion on energy expenditure and metabolism in a rat model of congestive heart failure cachexia.MethodsAdult female rats of the Sprague Dawley strain (n = 33) were used (11 pair-fed control, 12 ad libitum and 10, 1-sarcosine–angiotensin II-infused rats). Body weight, faecal excretion, feed intake (in grams), water intake (in milliliters) and urine excreted were recorded daily. The measurements were recorded in three different periods (4 days prior to surgery, “pre-infusion”; day of surgery and 5 days postsurgery, “infusion period”; days 7 to 14, “recovery” period). Different analytical methods were used to measure energy expenditure per period, uncoupling protein 3 mRNA expression, crude protein and adipose tissue body composition.ResultsDuring the infusion period, the SAR–Ang II group experienced rapid weight loss (p 0.05) in comparison to the ad libitum and pair-fed groups. The SAR–Ang II group displayed lower (p 0.05) body fat content (in percent) than the controls. There was also increased (p 0.05) uncoupling protein 3 (UCP3) mRNA expression in the SAR–Ang II group and pair-fed group when compared to the controls.ConclusionIn summary, the results suggest that SAR–Ang II infusion impairs appetite and decreases body weight by wasting predominantly adipose tissue, which may be due to elevated energy expenditure via mitochondrial uncoupling (UCP3 protein activity).

机译：摘要背景有无数的蛋白质负责调节能量消耗。血管紧张素II（Ang II）是肾素-血管紧张素系统的重要组成部分，它影响血压，并通过脂肪和肌肉代谢与恶病质和肥胖症相关。先前的研究表明，Ang II的直接作用是通过血管紧张素II 1型受体蛋白作用于大脑，从而影响食物摄入和能量消耗。本研究的目的是研究在充血性心力衰竭恶病质大鼠模型中1-sarcosine（SAR）-Ang II输注对能量消耗和代谢的影响。使用（11对喂食的对照，12只随意进食的和10只注入1-肌氨酸-血管紧张素II的大鼠）。每天记录体重，粪便排泄，饲料摄入（以克为单位），水摄入（以毫升为单位）和尿液排泄。在三个不同的时期记录测量值（手术前4天，“输液前”;手术日和手术后5天，“输液期”;第7至14天，“恢复”期）。结果：在输注期间，SAR-Ang II组与对照组相比，体重减轻迅速（p <0.05），采用了不同的分析方法来测量每个周期的能量消耗，解偶联蛋白3 mRNA表达，粗蛋白和脂肪组织的身体成分。随意和成对喂食的团体。 SAR–Ang II组的体脂含量（百分比）低于对照组（p <0.05）。与对照组相比，SAR–Ang II组和成对进食组的解偶联蛋白3（UCP3）mRNA表达也有所增加（p <0.05）。通过主要消耗脂肪组织降低体重，这可能是由于线粒体解偶联（UCP3蛋白活性）导致能量消耗增加。

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《Journal of Cachexia, Sarcopenia and Muscle》 |2014年第3期|共8页
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Cichello S. A.; Schuijers J.; Weisinger R. S.;
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1. 1-Sarcosine–angiotensin II infusion effects on food intake, weight loss, energy expenditure, and skeletal muscle UCP3 gene expression in a rat model [J] . S. A. Cichello, R. S. Weisinger, J. Schuijers, Journal of Cachexia, Sarcopenia and Muscle . 2014,第3期

机译：1-Sarcosine-血管紧张素II输注对大鼠模型中食物摄入，体重减轻，能量消耗和骨骼肌UCP3基因表达的影响
2. The contraction induced increase in gene expression of peroxisome proliferator-activated receptor (PPAR)-gamma coactivator 1 alpha (PGC-1 alpha), mitochondrial uncoupling protein 3 (UCP3) and hexokinase II (HKII) in primary rat skeletal muscle cells [J] . Silveira LR, Pilegaard H, Kusuhara K, Biochimica et biophysica acta. Molecular cell research . 2006,第9期

机译：收缩诱导原代大鼠骨骼肌细胞中过氧化物酶体增殖物激活受体（PPAR）-γ共激活因子1 alpha（PGC-1 alpha），线粒体解偶联蛋白3（UCP3）和己糖激酶II（HKII）基因表达的增加。
3. Feed restriction up-regulates uncoupling protein 3 (UCP3) gene expression in heart and red muscle tissues of gilthead sea bream (Sparus aurata L.). New insights in substrate oxidation and energy expenditure. [J] . Bermejo-Nogales A., Benedito-Palos L., Calduch-Giner J.A., Comparative biochemistry and physiology, Part A. Molecular and integrative physiology . 2011,第3期

机译：进食限制上调了金头鲷（Sparus aurata L.）的心脏和红色肌肉组织中解偶联蛋白3（UCP3）基因的表达。基板氧化和能量消耗的新见解。
4. Decellularized skeletal muscle with autologous minced muscle improves regeneration after volumetric muscle loss [C] . Ben Kasukonis, John Kim, Tyrone Washington, World biomaterials congress . 2016

机译：具有自体碎肉的去细胞骨骼肌可改善容积性肌肉丢失后的再生
5. Angiotensin II regulation of skeletal muscle regeneration, growth and satellite cell function. [D] . Johnston, Adam P.W. 2011

机译：血管紧张素II调节骨骼肌的再生，生长和卫星细胞功能。
6. 1-Sarcosine–angiotensin II infusion effects on food intake weight loss energy expenditure and skeletal muscle UCP3 gene expression in a rat model [O] . S. A. Cichello, R. S. Weisinger, J. Schuijers, 2014

机译：1-Sarcosine-Angiotensin II输注对大鼠模型中食物摄入体重减轻能量消耗和骨骼肌UCP3基因表达的影响
7. 1-Sarcosine-angiotensin II infusion effects on food intake, weight loss, energy expenditure, and skeletal muscle UCP3 gene expression in a rat model [O] . S. A. Cichello, R. S. Weisinger, J. Schuijers, 2014

机译：1-Sarcosine-angiotensin II输液对大鼠模型中的食物摄入，减肥，能量消耗和骨骼肌UCP3基因表达的影响

1‐Sarcosine–angiotensin II infusion effects on food intake, weight loss, energy expenditure, and skeletal muscle UCP3 gene expression in a rat model

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