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用抗杜氏肌营养不良肽抗体对骨骼肌和心肌表面膜进行免疫染色。

Immunostaining of skeletal and cardiac muscle surface membrane with antibody against Duchenne muscular dystrophy peptide.

作者信息

Arahata K, Ishiura S, Ishiguro T, Tsukahara T, Suhara Y, Eguchi C, Ishihara T, Nonaka I, Ozawa E, Sugita H

机构信息

National Institute of Neuroscience, NCNP, Tokyo, Japan.

出版信息

Nature. 1988 Jun 30;333(6176):861-3. doi: 10.1038/333861a0.

Abstract

Duchenne muscular dystrophy (DMD) is a debilitating X-linked muscle disease. We have used sequence information from complementary DNA clones, derived from the gene that is deleted in DMD patients, to generate an antiserum that stains the surface membrane of intact human and mouse skeletal muscle, but not that of DMD patients and mdx mice. Here we identify the protein reacting with this antiserum as a single component of relative molecular mass 210,000 (Mr = 210K) that fractionates with a low-ionic strength extract of intact human and mouse skeletal muscle. It is therefore distinct from the 400 K protein found in the heavy microsomal fraction of normal muscle and identified as a putative product of the DMD gene. We also analyse further the disease specificity of the antiserum. Positive staining is seen in normal controls, and in samples from patients with a wide range of muscular dystrophies other than DMD. Becker muscular dystrophy, which is allelically related to DMD, was the only other exception, and gave a sporadic staining pattern. The demonstration of a specific defect in the surface membrane of DMD muscle fibres substantiates the hypothesis that membrane lesions may initiate muscle degradation in DMD.

摘要

杜兴氏肌肉营养不良症(DMD)是一种使人衰弱的X连锁肌肉疾病。我们利用从DMD患者缺失的基因中获得的互补DNA克隆的序列信息,制备了一种抗血清,该抗血清可对完整的人类和小鼠骨骼肌的表面膜进行染色,但不能对DMD患者和mdx小鼠的表面膜进行染色。在这里,我们确定与这种抗血清反应的蛋白质是一种相对分子质量为210,000(Mr = 210K)的单一成分,它可从完整的人类和小鼠骨骼肌的低离子强度提取物中分离出来。因此,它与在正常肌肉的重微粒体部分中发现的400K蛋白质不同,后者被鉴定为DMD基因的推定产物。我们还进一步分析了该抗血清的疾病特异性。在正常对照以及来自除DMD之外的多种肌肉营养不良症患者的样本中均可见阳性染色。与DMD等位基因相关的贝克氏肌肉营养不良症是唯一的另一个例外,呈现出散在的染色模式。DMD肌纤维表面膜存在特异性缺陷的证明证实了膜损伤可能引发DMD肌肉退化的假说。

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