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Oral administration of creatine monohydrate retards progression of motor neuron disease in the wobbler mouse

机译:口服肌酸一水合物可延缓摆动小鼠的运动神经元疾病进展

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BACKGROUND AND AIMS: Creatine has a neuroprotective effect in mutant superoxide dismutase (G93A) transgenic mice, an animal model of motor neuron disease (MND). Treatment with creatine monohydrate enhances muscle strength in patients with neuromuscular disorders. The purpose of our study was to determine whether administration of creatine monohydrate can attenuate progressive disease in wobbler mice. METHODS: After an initial diagnosis of disease at the age of 3-4 weeks, creatine monohydrate (5 or 50 mg/kg, po) or vehicle was given to wobbler mice daily for 4 weeks in a blinded fashion. We compared symptomatic and neuropathological assessments among the three groups. RESULTS: Creatine levels in biceps muscles were increased by approximately 20% following administration of higher-dose creatine monohydrate. In comparison with vehicle, treatment with higher doses of creatine monohydrate potentiated grip strength, attenuated forelimb contracture and increased the weight of biceps muscles. Mice treated with higher doses of creatine monohydrate showed retarded denervation muscle atrophy in the biceps muscles and reduced degeneration of the spinal motor neurons. Thus, oral administration of creatine monohydrate delayed the progression of disease in wobbler mice. CONCLUSION: Our results indicate that this molecule may have therapeutic potential in human motor neuropathy or MND.
机译:背景与目的:肌酸在突变型超氧化物歧化酶(G93A)转基因小鼠中具有神经保护作用,后者是运动神经元疾病(MND)的动物模型。一水肌酸治疗可增强神经肌肉疾病患者的肌肉力量。我们研究的目的是确定肌酸一水合物的使用是否可以减轻摇摆小鼠的疾病进展。方法:在最初诊断为3-4周龄的疾病后,每天向摇摇晃晃的小鼠每天注射一水肌酸(5或50 mg / kg,口服)或溶媒,以盲法服用4周。我们比较了三组的症状和神经病理学评估。结果:服用高剂量肌酸一水合物后,二头肌肌肉中的肌酸水平增加了约20%。与赋形剂相比,用更高剂量的一水化肌酸进行治疗可增强握力,减弱前肢挛缩并增加二头肌的重量。用较高剂量的一水合肌酸水合物治疗的小鼠在二头肌中显示出神经支配性肌肉萎缩的延迟和脊髓运动神经元变性的减少。因此,口服肌酸一水合物延迟了摆动小鼠的疾病进展。结论:我们的结果表明该分子可能在人类运动神经病或MND中具有治疗潜力。

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