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Enhanced tethered-flight duration and locomotor activity byoverexpression of the human gene SOD1 in Drosophilamotorneurons

机译:通过以下方式增强了系留飞行的持续时间和运动能力果蝇中人类基因SOD1的过表达运动神经元

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摘要

Mutation of the human gene superoxide dismutase (hSOD1) is associated with the fatal neurodegenerative disease familial amyotrophic lateral sclerosis (Lou Gehrig’s disease). Selective overexpression of hSOD1 in Drosophila motorneurons increases lifespan to 140% of normal. The current study was designed to determine resistance to lifespan decline and failure of sensorimotor functions by overexpressing hSOD1 in Drosophila‘s motorneurons. First, we measured the ability to maintain continuous flight and wingbeat frequency (WBF) as a function of age (5 to 50 days). Flies overexpressing hSOD1 under the D42-GAL4 activator were able to sustain flight significantly longer than controls, with the largest effect observed in the middle stages of life. The hSOD1-expressed line also had, on average, slower wingbeat frequencies in late, but not early life relative to age-matched controls. Second, we examined locomotor (exploratory walking) behavior in late life when flies had lost the ability to fly (age ≥ 60 d). hSOD1-expressed flies showed significantly more robust walking activity relative to controls. Findings show patterns of functional decline dissimilar to those reported for other life-extended lines, and suggest that thehSOD1 gene not only delays death but enhances sensorimotorabilities critical to survival even in late life.
机译:人类基因超氧化物歧化酶(hSOD1)的突变与致命性神经退行性疾病家族性肌萎缩性侧索硬化症(Lou Gehrig病)有关。果蝇运动神经元中hSOD1的选择性过表达将寿命延长至正常值的140%。当前的研究旨在通过在果蝇的运动神经元中过表达hSOD1来确定对寿命下降和感觉运动功能衰竭的抵抗力。首先,我们根据年龄(5至50天)测量了保持连续飞行和机翼拍打频率(WBF)的能力。在D42-GAL4激活剂下过表达hSOD1的果蝇能够比对照维持更长的飞行时间,在生命的中期阶段观察到最大的影响。与年龄相匹配的对照组相比,表达hSOD1的品系在后期(但不是早期)平均也具有较慢的翅膀频率。其次,我们研究了晚年苍蝇失去飞行能力(年龄≥60 d)时的运动(探索性步行)行为。表达hSOD1的果蝇显示出比对照组明显更健壮的步行活动。调查结果显示功能下降的模式与其他寿命延长线所报告的模式不同,并表明hSOD1基因不仅延迟死亡,而且增强感觉运动甚至对于晚年生存至关重要的能力。

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