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首页> 外文期刊>Molecular biology of the cell >A Highlights from MBoC Selection: The rod domain is not essential for the function of plectin in maintaining tissue integrity
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A Highlights from MBoC Selection: The rod domain is not essential for the function of plectin in maintaining tissue integrity

机译:MBoC选择的亮点:杆结构域对于Plectin维持组织完整性的功能不是必需的

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Epidermolysis bullosa simplex associated with late-onset muscular dystrophy (EBS-MD) is an autosomal recessive disorder resulting from mutations in the plectin gene. The majority of these mutations occur within the large exon 31 encoding the central rod domain and leave the production of a low-level rodless plectin splice variant unaffected. To investigate the function of the rod domain, we generated rodless plectin mice through conditional deletion of exon 31. Rodless plectin mice develop normally without signs of skin blistering or muscular dystrophy. Plectin localization and hemidesmosome organization are unaffected in rodless plectin mice. However, superresolution microscopy revealed a closer juxtaposition of the C-terminus of plectin to the integrin β4 subunit in rodless plectin keratinocytes. Wound healing occurred slightly faster in rodless plectin mice than in wild-type mice, and keratinocytes migration was increased in the absence of the rod domain. The faster migration of rodless plectin keratinocytes is not due to altered biochemical properties because, like full-length plectin, rodless plectin is a dimeric protein. Our data demonstrate that rodless plectin can functionally compensate for the loss of full-length plectin in mice. Thus the low expression level of plectin rather than the absence of the rod domain dictates the development of EBS-MD.
机译:与迟发性肌营养不良症(EBS-MD)相关的大疱表皮松解症是一种由于Plectin基因突变导致的常染色体隐性遗传疾病。这些突变中的大多数发生在编码中心杆结构域的大外显子31内,并且不影响低水平无杆凝集素剪接变体的产生。为了研究杆结构域的功能,我们通过有条件地缺失外显子31产生了无杆选择素小鼠。无杆选择素小鼠正常发育,没有皮肤起泡或肌营养不良的迹象。在无杆的plectin小鼠中,lectin的定位和半染色体的组织不受影响。然而,超高分辨率显微镜显示无杆状凝集素角质形成​​细胞中凝集素的C末端与整联蛋白β4亚基更紧密地并置。无杆血球凝集素小鼠的伤口愈合比野生型小鼠稍快,并且在没有杆域的情况下角质形成细胞迁移增加。无杆凝集素角质形成​​细胞的更快迁移不是由于生化特性的改变,因为像全长凝集素一样,无杆凝集素是二聚体蛋白。我们的数据表明,无杆凝集素可以在功能上补偿小鼠体内全长凝集素的损失。因此,凝集素的低表达水平而不是杆结构域的缺乏决定了EBS-MD的发展。

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