巨大轴索性神经病:一种影响细胞骨架组织的条件性突变。
Giant axonal neuropathy: a conditional mutation affecting cytoskeletal organization.
作者信息
Klymkowsky M W, Plummer D J
出版信息
J Cell Biol. 1985 Jan;100(1):245-50. doi: 10.1083/jcb.100.1.245.
Abstract
Giant axonal neuropathy (GAN) results from autosomal recessive mutations (gan-) that affect cytoskeletal organization; specifically, intermediate filaments (IFs) are found collapsed into massive bundles in a variety of different cell types. We studied the gan- fibroblast lines WG321 and WG139 derived from different GAN patients. Although previous studies implied that the gan- IF phenotype was constitutive, we find that it is conditional. That is, when cells were grown under the permissive condition of medium containing over 2% fetal calf serum, most cells had normal IF organization. IF bundles formed when gan- cells were transferred to the nonpermissive condition of low (0.1%) serum. Microtubule organization appeared normal in the presence or absence of serum. The effect of serum starvation was largely blocked or reversed by the addition of BSA to the culture media. We found no evidence that the gan- phenotype depends upon progress through the cell cycle. We discuss the possible role of serum effects in the etiology of GAN and speculate as to the molecular nature of the gan- defect.
摘要
巨轴索神经病(GAN)由常染色体隐性突变(gan-)引起,这些突变影响细胞骨架组织;具体而言,在多种不同细胞类型中发现中间丝(IFs)塌陷成巨大束状。我们研究了源自不同GAN患者的gan-成纤维细胞系WG321和WG139。尽管先前的研究表明gan-IF表型是组成性的,但我们发现它是条件性的。也就是说,当细胞在含有超过2%胎牛血清的培养基的允许条件下生长时,大多数细胞具有正常的IF组织。当gan-细胞转移到低(0.1%)血清的非允许条件下时,IF束形成。在有或无血清的情况下,微管组织看起来正常。通过向培养基中添加牛血清白蛋白(BSA),血清饥饿的影响在很大程度上被阻断或逆转。我们没有发现证据表明gan-表型取决于细胞周期进程。我们讨论了血清效应在GAN病因学中的可能作用,并推测gan-缺陷的分子性质。
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