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再生与萎缩骨骼肌、肌病及横纹肌瘤性肿瘤中α-肌动蛋白的心脏同工型:一项使用单克隆抗体的免疫组织化学研究

The cardiac isoform of alpha-actin in regenerating and atrophic skeletal muscle, myopathies and rhabdomyomatous tumors: an immunohistochemical study using monoclonal antibodies.

作者信息

Moll Roland, Holzhausen Hans-Jürgen, Mennel Hans-Dieter, Kuhn Caecilia, Baumann Renate, Taege Christiane, Franke Werner W

机构信息

Institute of Pathology, Philipp University of Marburg, Baldingerstrasse, D-35033 Marburg, Germany.

出版信息

Virchows Arch. 2006 Aug;449(2):175-91. doi: 10.1007/s00428-006-0220-7. Epub 2006 May 20.

DOI:10.1007/s00428-006-0220-7
PMID:16715231
Abstract

The two sarcomeric isoforms of actins, cardiac and skeletal muscle alpha-actin, are highly homologous so that their immunohistochemical distinction is extremely difficult. Taking advantage of monoclonal antibodies distinguishing the two conservative amino acid exchanges near the aminoterminus, we have performed an extended immunohistochemical analysis of the cardiac alpha-actin (CAA) isoform in normal, regenerating, diseased and neoplastic human muscle tissues. Intense and uniform CAA staining is seen in fetal and adult myocardium and in fetal skeletal muscle while adult skeletal muscle is essentially negative, except for muscle spindle myocytes and a few scattered muscle fibres with overall reduced diameter. By contrast, CAA synthesis is markedly induced in regenerating skeletal muscle cells, in Duchenne muscular dystrophy and upon degenerative atrophy. CAA has also been detected in certain vascular and visceral smooth muscle cells. Among tumors, CAA has consistently been seen in rhabdomyosarcomas and rhabdomyomatous cells of nephroblastomas, whereas, smooth muscle tumors have shown only occasional staining. While the synthesis of this actin isoform is less restricted than previously thought, monoclonal antibodies against CAA provide a well-defined, reliable and sensitive diagnostic tool for the definition and detection of aberrant differentiation in diseased skeletal muscle and of striated muscle differentiation in rhabdomyosarcomas.

摘要

肌动蛋白的两种肌节同工型,即心肌和骨骼肌α-肌动蛋白,高度同源,因此通过免疫组织化学方法区分它们极为困难。利用可区分氨基末端附近两个保守氨基酸交换的单克隆抗体,我们对正常、再生、患病和肿瘤性人类肌肉组织中的心肌α-肌动蛋白(CAA)同工型进行了广泛的免疫组织化学分析。在胎儿和成人心肌以及胎儿骨骼肌中可见强烈且均匀的CAA染色,而除肌梭肌细胞和少数直径总体减小的散在肌纤维外,成人骨骼肌基本呈阴性。相比之下,在再生骨骼肌细胞、杜兴氏肌营养不良症以及退行性萎缩时,CAA合成明显诱导。在某些血管和内脏平滑肌细胞中也检测到了CAA。在肿瘤中,在横纹肌肉瘤和肾母细胞瘤的横纹肌样细胞中一直可见CAA,而平滑肌肿瘤仅偶尔有染色。虽然这种肌动蛋白同工型的合成限制比以前认为的要少,但针对CAA的单克隆抗体为定义和检测患病骨骼肌中的异常分化以及横纹肌肉瘤中的横纹肌分化提供了一种明确、可靠且灵敏的诊断工具。

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