Gabreëls-Festen A A, Hoogendijk J E, Meijerink P H, Gabreëls F J, Bolhuis P A, van Beersum S, Kulkens T, Nelis E, Jennekens F G, de Visser M, van Engelen B G, Van Broeckhoven C, Mariman E C
Institute of Neurology, University Hospital Nijmegen, The Netherlands.
Neurology. 1996 Sep;47(3):761-5. doi: 10.1212/wnl.47.3.761.
In seven unrelated patients with a demyelinating motor and sensory neuropathy, we found mutations in exons 2 and 3 of the P0 gene. Morphologic examination of sural nerve biopsy specimens showed a demyelinating process with onion bulb formation in all cases. In four patients, ultrastructural examination demonstrated uncompacted myelin in 23 to 68% of the myelinated fibers, which is in agreement with the widely accepted function of P0 as a homophilic adhesion molecule. Three patients showed normal compact myelin, but morphology was dominated by the abundant occurrence of focally folded myelin. The two divergent pathologic phenotypes exemplify that some mutations act differently on P0 protein formation or function than others, which is probably determined by site and nature of the mutation in the P0 gene.
在7例患有脱髓鞘性运动和感觉神经病的非亲属患者中,我们发现P0基因第2和第3外显子存在突变。腓肠神经活检标本的形态学检查显示,所有病例均有脱髓鞘过程并伴有洋葱球形成。在4例患者中,超微结构检查显示23%至68%的有髓纤维存在髓鞘疏松,这与广泛认可的P0作为同种亲和黏附分子的功能相符。3例患者的致密髓鞘正常,但形态学上以大量局灶性折叠髓鞘为主。这两种不同的病理表型表明,一些突变对P0蛋白形成或功能的作用与其他突变不同,这可能由P0基因中突变的位点和性质决定。
