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中风后的肌肉分子表型与步态速度相关。

Muscle molecular phenotype after stroke is associated with gait speed.

作者信息

De Deyne Patrick G, Hafer-Macko Charlene E, Ivey Frederick M, Ryan Alice S, Macko Richard F

机构信息

Departments of Physical Therapy and Rehabilitation Science, University of Maryland School of Medicine, Baltimore, Maryland, USA.

出版信息

Muscle Nerve. 2004 Aug;30(2):209-15. doi: 10.1002/mus.20085.

Abstract

The disability of patients after stroke is generally attributed to upper motor neuron defects, but secondary changes in paretic muscle may enhance the disability. We analyzed the molecular phenotype and metabolic profile of the paretic and nonparetic vastus lateralis (VL) and we measured the severity of gait deficit in 13 patients at least 6 months after ischemic stroke. The results showed a significant increase in the proportion of fast myosin heavy chain (MHC, 68 +/- 14%) in the paretic compared to the nonparetic VL (50 +/- 13%). The specific activity of citrate synthase and glyceraldehyde phosphodehydrogenase was not significantly different between the two sides. The proportion of fast MHC was inversely associated with severity of gait deficit indexed by self-selected walking speed in the paretic leg, but not the nonparetic leg. Our findings demonstrate significant and potentially modifiable secondary biologic changes in hemiparetic muscle phenotype that may contribute to the disability of stroke.

摘要

中风后患者的残疾通常归因于上运动神经元缺陷,但瘫痪肌肉的继发性变化可能会加重残疾程度。我们分析了瘫痪侧和非瘫痪侧股外侧肌(VL)的分子表型和代谢谱,并测量了13例缺血性中风至少6个月后的患者步态缺陷的严重程度。结果显示,与非瘫痪侧VL(50±13%)相比,瘫痪侧快速肌球蛋白重链(MHC,68±14%)的比例显著增加。两侧柠檬酸合酶和甘油醛磷酸脱氢酶的比活性无显著差异。快速MHC的比例与以患侧腿自选步行速度为指标的步态缺陷严重程度呈负相关,而非患侧腿则无此关系。我们的研究结果表明,偏瘫肌肉表型存在显著且可能可改变的继发性生物学变化,这可能导致中风后的残疾。

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