髓磷脂蛋白零基因中的两个新型错义突变导致2型夏科-马里-图斯病和德热里纳-索塔斯综合征。
Two novel missense mutations in the myelin protein zero gene causes Charcot-Marie-Tooth type 2 and Déjérine-Sottas syndrome.
作者信息
Braathen Geir J, Sand Jette C, Russell Michael B
机构信息
Faculty Division Akershus University Hospital, University of Oslo, 1474 Nordbyhagen, Oslo, Norway.
出版信息
BMC Res Notes. 2010 Apr 12;3:99. doi: 10.1186/1756-0500-3-99.
BACKGROUND
The Charcot-Marie-Tooth (CMT) phenotype caused by mutation in the myelin protein zero (MPZ) gene varies considerably, from early onset and severe forms to late onset and milder forms. The mechanism is not well understood. The myelin protein zero (P0) mediates adhesion in the spiral wraps of the Schwann cell's myelin sheath. The crystalline structure of the extracellular domain of the myelin protein zero (P0ex) is known, while the transmembrane and intracellular structure is unknown.
FINDINGS
One novel missense mutation caused a milder late onset CMT type 2, while the second missense mutation caused a severe early onset phenotype compatible with Déjérine-Sottas syndrome.
CONCLUSIONS
The phenotypic variation caused by different missense mutations in the MPZ gene is likely caused by different conformational changes of the MPZ protein which affects the functional tetramers. Severe changes of the MPZ protein cause dysfunctional tetramers and predominantly uncompacted myelin, i.e. the severe phenotypes congenital hypomyelinating neuropathy and Déjérine-Sottas syndrome, while milder changes cause the phenotypes CMT type 1 and 2.
背景
髓鞘蛋白零(MPZ)基因突变导致的夏科-马里-图斯(CMT)表型差异很大,从早发型和严重型到晚发型和轻型。其机制尚不清楚。髓鞘蛋白零(P0)介导施万细胞髓鞘螺旋包裹中的黏附。髓鞘蛋白零细胞外结构域(P0ex)的晶体结构已知,而跨膜和细胞内结构未知。
研究结果
一个新的错义突变导致了较轻的晚发型CMT 2型,而第二个错义突变导致了与德热里纳-索塔斯综合征相符的严重早发型表型。
结论
MPZ基因不同错义突变引起的表型变异可能是由于MPZ蛋白不同的构象变化影响了功能性四聚体。MPZ蛋白的严重变化导致功能失调的四聚体和主要未紧密包裹的髓鞘,即严重表型先天性髓鞘形成不良性神经病和德热里纳-索塔斯综合征,而较轻的变化则导致CMT 1型和2型表型。
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