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对[3H]哇巴因与人骨骼肌低温恒温器切片结合的定量测量。

Quantitative measurement of [3H]ouabain binding to human skeletal muscle cryostat sections.

作者信息

Desaiah D, Mishra S K, Hobson M

出版信息

J Neurol Sci. 1981 Sep;51(3):457-64. doi: 10.1016/0022-510x(81)90122-2.

Abstract

The etiopathogenesis of myotonic muscular dystrophy is thought to involve a basic defect in muscle membrane. Biochemical investigations of human muscle membrane have been hampered by difficulty in obtaining large quantities of muscle at biopsy for the preparation of sarcolemma. We have determined [3H]ouabain binding to normal and myotonic dystrophy human skeletal muscle by using cryostat sections. The binding increased with increase in number of tissue sections (protein) and in concentrations of [3H]ouabain, ATP and Na+. The binding of [3H]ouabain in myotonic dystrophy patients was 2-3 fold higher than in normal and disease controls. Kinetic analysis revealed that the increased binding of ouabain to myotonic tissue sections was independent of low-affinity sites directed by ATP and Na+. These findings provide further evidence for the involvement of membrane abnormalities in myotonic muscular dystrophy.

摘要

强直性肌营养不良的发病机制被认为涉及肌膜的基本缺陷。对人肌膜的生化研究因活检时难以获取大量肌肉以制备肌膜而受到阻碍。我们通过使用冷冻切片机切片测定了[3H]哇巴因与正常和强直性肌营养不良患者的人骨骼肌的结合情况。结合量随组织切片数量(蛋白质)以及[3H]哇巴因、ATP和Na+浓度的增加而增加。[3H]哇巴因在强直性肌营养不良患者中的结合量比正常人和疾病对照者高2至3倍。动力学分析表明,哇巴因与强直性肌营养不良组织切片结合量的增加与由ATP和Na+介导的低亲和力位点无关。这些发现为膜异常参与强直性肌营养不良提供了进一步的证据。

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