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肌萎缩侧索硬化症大鼠模型疾病发作和进展中的性别二态性。

Sexual dimorphism in disease onset and progression of a rat model of ALS.

作者信息

Suzuki Masatoshi, Tork Craig, Shelley Brandon, McHugh Jacalyn, Wallace Kyle, Klein Sandra M, Lindstrom Mary J, Svendsen Clive N

机构信息

Stem Cell Research Program in Neuroscience, The Waisman Center and Department of Anatomy, University of Wisconsin-Madison, Madison, WI 53705-2280, USA.

出版信息

Amyotroph Lateral Scler. 2007 Feb;8(1):20-5. doi: 10.1080/17482960600982447.

Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease causing the progressive loss of brain and spinal cord motor neurons. The exact etiology of ALS is still uncertain, but males have consistently been shown to be at a higher risk for the disease than females. Recently, transgenic rats overexpressing mutant forms of the human SOD1 (hSOD1) gene have been established as a valuable disease model of ALS. Here we show that sexual dimorphism in disease onset is also observed in hSOD1G93A transgenic rats. Disease onset was consistently earlier in male than in female hSOD1G93A rats. We also found that hSOD1G93A male rats lost weight more rapidly following disease onset compared to hSOD1G93A females. Furthermore, we tested locomotor function using the Basso-Beattie-Bresnahan (BBB) rating scale and a beam walking test. We found that motor dysfunction started earlier in males than in females but progressed similarly in the two sexes. These results have important implications for future experimentation and therapeutic development using the rat model of ALS.

摘要

肌萎缩侧索硬化症(ALS)是一种致命的神经退行性疾病,会导致大脑和脊髓运动神经元逐渐丧失。ALS的确切病因仍不确定,但一直以来男性患该疾病的风险高于女性。最近,过表达人类超氧化物歧化酶1(hSOD1)基因突变形式的转基因大鼠已被确立为一种有价值的ALS疾病模型。在此我们表明,在hSOD1G93A转基因大鼠中也观察到疾病发病的性别差异。hSOD1G93A雄性大鼠的疾病发病始终早于雌性大鼠。我们还发现,与hSOD1G93A雌性大鼠相比,hSOD1G93A雄性大鼠在疾病发病后体重下降更快。此外,我们使用巴索-贝蒂-布雷斯纳汉(BBB)评分量表和横梁行走测试对运动功能进行了测试。我们发现,运动功能障碍在雄性大鼠中比在雌性大鼠中出现得更早,但在两性中进展相似。这些结果对未来使用ALS大鼠模型进行的实验和治疗开发具有重要意义。

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