首页> 美国卫生研究院文献>Physiological Reports >Elevated GLUT4 and glycogenin protein abundance correspond to increased glycogen content in the soleus muscle of mdx mice with no benefit associated with taurine supplementation
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Elevated GLUT4 and glycogenin protein abundance correspond to increased glycogen content in the soleus muscle of mdx mice with no benefit associated with taurine supplementation

机译:GLUT4和糖原蛋白蛋白含量的升高对应于mdx小鼠比目鱼肌中糖原含量的增加而与牛磺酸补充剂无关

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摘要

Duchenne muscular dystrophy (DMD) patients and the dystrophic mdx mouse have an elevated demand for ATP requiring processes, including Ca2+ regulation and skeletal muscle regeneration. As a key substrate for cellular ATP production, altered glycogen metabolism may contribute significantly to dystrophic pathology and explain reports of mild glucose intolerance. We compare the soleus and extensor digitorum longus (EDL) muscles of the mdx mouse during active muscle necrosis (at 28 days) and at 70 days where pathology is stable. We further investigate the impact of taurine (tau) on dystrophic glycogen metabolism to identify if the benefit seen with tau in a previous study (Barker et al. ) was in part owed to altered glycogen handling. The soleus muscle of 28‐ and 70‐day‐old mdx mice had elevated glucose transporter type 4 (GLUT4), glycogenin protein abundances and glycogen content compared to WT (C57BL10/ScSn) controls. Mdx tau mice exhibited modestly reduced glycogen compared to their respective mdx group. The EDL muscle of 28 days mdx tau mice had a ~70% increase in glycogenin protein abundance compared to the mdx but 50% less glycogen content. A twofold greater phosphorylated glycogen synthase (p‐GS) and glycogen phosphorylase (p‐GP) protein abundance was observed in the 70‐day‐old mdx soleus muscle than in the 28‐day‐old mdx soleus muscle. Glycogen debranching enzyme (GDE) protein abundance was elevated in both 28‐ and 70‐day‐old mdx soleus muscles compared to WT controls. We identified an increase in proteins associated with glucose uptake and utilization specific to the predominantly slow‐twitch soleus muscle of mdx mice regardless of age and that taurine affords no obvious benefit to glycogen metabolism in the mdx mouse.
机译:Duchenne肌营养不良症(DMD)患者和营养不良的mdx小鼠对ATP需求过程(包括Ca 2 + 调节和骨骼肌再生)的需求增加。作为细胞ATP产生的关键底物,糖原代谢的改变可能显着促进营养不良性病理,并解释了轻度葡萄糖不耐受的报道。我们比较了mdx小鼠在活动性肌肉坏死期间(第28天)和第70天病理稳定的比目鱼肌和比趾长肌(EDL)肌肉。我们将进一步研究牛磺酸(tau)对营养不良性糖原代谢的影响,以确定先前研究(Barker等)中使用tau的益处是否部分归因于糖原处理的改变。与WT(C57BL10 / ScSn)对照相比,28和70天龄mdx小鼠的比目鱼肌具有升高的4型葡萄糖转运蛋白(GLUT4),糖原蛋白蛋白丰度和糖原含量。与它们各自的mdx组相比,Mdx tau小鼠显示出适度降低的糖原。与mdx相比,28天mdx tau小鼠的EDL肌肉糖原蛋白蛋白质丰度增加了约70%,但糖原含量却减少了50%。在70天的mdx比目鱼肌中发现的磷酸化糖原合酶(p-GS)和糖原磷酸化酶(p-GP)蛋白的丰度是28天的mdx比目鱼肌的两倍。与WT对照相比,在28天和70天的mdx比目鱼肌中糖原解支酶(GDE)蛋白的丰度都增加了。我们发现,无论年龄大小,与特定于mdx小鼠的主要慢抽动比目鱼肌相关的葡萄糖摄取和利用相关的蛋白质的增加,并且牛磺酸对mdx小鼠的糖原代谢没有明显的好处。

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