Evans D G, Trueman L, Wallace A, Collins S, Strachan T
Department of Medical Genetics, St Mary's Hospital, Manchester, UK.
J Med Genet. 1998 Jun;35(6):450-5. doi: 10.1136/jmg.35.6.450.
Blood samples from 125 unrelated families with classical type 2 neurofibromatosis (NF2) with bilateral vestibular schwannomas have been analysed for mutations in the NF2 gene. A further 17 families fulfilling modified criteria for NF2 have also been analysed. Causative mutations have been identified in 54 (43%) classical families and six (35%) of those fulfilling modified criteria. Forty-two cases from 38 families with truncating mutations had an average age at onset of symptoms of 19 years and diagnosis at 22.4 years. Fifty-one cases from 16 families with splice site mutations (15 from six), missense mutations (18 from six), and large deletions (18 from five) had an average age of onset of 27.8 years and at diagnosis of 33.4 years. Subjects with truncating mutations were significantly more likely to have symptoms before 20 years of age (p<0.001) and to develop at least two symptomatic CNS tumours in addition to vestibular schwannoma before 30 years (p<0.001). There were also significantly fewer multigenerational families with truncating mutations. Four further truncating mutations were in mosaic form and were associated with milder disease than other similar mutations. This large study has confirmed the previous impression that truncating mutations are associated with severe disease, but caution has to be exercised in using mutation type to predict disease course.
对125个患有双侧前庭神经鞘瘤的典型2型神经纤维瘤病(NF2)的无关家庭的血样进行了NF2基因突变分析。另外还分析了17个符合NF2修改标准的家庭。在54个(43%)典型家庭和6个(35%)符合修改标准的家庭中发现了致病突变。来自38个有截短突变家庭的42例患者症状出现的平均年龄为19岁,诊断时平均年龄为22.4岁。来自16个家庭的51例患者,其中有剪接位点突变(6个家庭中的15例)、错义突变(6个家庭中的18例)和大片段缺失(5个家庭中的18例),症状出现的平均年龄为27.8岁,诊断时平均年龄为33.4岁。有截短突变的患者在20岁之前出现症状的可能性显著更高(p<0.001),并且在30岁之前除前庭神经鞘瘤外还至少发生两个有症状的中枢神经系统肿瘤的可能性也更高(p<0.001)。有截短突变的多代家庭也明显更少。另外有4个截短突变呈镶嵌形式,与其他类似突变相比,疾病症状较轻。这项大型研究证实了之前的印象,即截短突变与严重疾病相关,但在使用突变类型预测疾病进程时必须谨慎。
