Drouet A, Le Moigne F, Salamé D, Quesnel L, Motolese C, des Portes V, Guilloton L, Pinson S
Service de neurologie, HIA Desgenettes, 108, boulevard Pinel, 69275 Lyon cedex 3, France; Centre de compétence neurofibromatose, Rhône-Alpes-Auvergne, centre Léon Bérard, 28, rue Laënnec, 69373 Lyon cedex 08, France.
Service de radiologie, HIA Desgenettes, 108, boulevard Pinel, 69275 Lyon cedex 3, France.
Arch Pediatr. 2014 Nov;21(11):1233-40. doi: 10.1016/j.arcped.2014.08.031. Epub 2014 Oct 22.
Neurofibromatosis type 2 (NF2) is a rare dominantly inherited disease. Its clinical presentation can be completely different in children and adults and early diagnosis is often difficult. The NF2 gene molecular analysis can help for diagnosis, but its result can be negative in case of NF2 mosaicism.
We report the case of a 43-year-old man who had developed a severe phenotype with bilateral vestibular schwannomas at 19 years of age. His son presented a retinal hamartoma with loss of vision in his right eye at 2 months of age. At 9 years of age, asymptomatic schwannomas of the cranial nerves were discovered: cranial nerves X (left), XI (left), and VIII (bilateral). Partial constitutional NF2 deletion (from exons 2-7) was detected in his son. The deletion was not detectable in the DNA blood of his father and we strongly suspect a mosaic form of NF2.
Ophthalmological manifestations can be the initial sign of NF2 in childhood. These features must be actively sought during the first year of life in individuals at risk of NF2. NF2 mosaicism is often described as a mild form of NF2 with a very low risk of transmission to the carrier's children. We show that NF2 mosaicism can sometimes develop severe NF2 symptoms and we confirm that the transmission risk to the offspring depends on the proportion of zygotes carrying the mutation. NF2 remains a life-limiting and life-spoiling condition. Early diagnosis is necessary to prevent complications and the follow-up of NF2 patients must be organized throughout life in specialty centers.
2型神经纤维瘤病(NF2)是一种罕见的常染色体显性遗传病。其临床表现因儿童和成人而异,早期诊断往往困难。NF2基因分子分析有助于诊断,但在NF2嵌合体情况下其结果可能为阴性。
我们报告了一名43岁男性的病例,他在19岁时出现了双侧前庭神经鞘瘤的严重表型。他的儿子在2个月大时出现视网膜错构瘤并伴有右眼视力丧失。9岁时,发现其存在无症状的颅神经神经鞘瘤:第X对(左侧)、第XI对(左侧)和第VIII对(双侧)颅神经。在他儿子身上检测到部分体质性NF2缺失(外显子2 - 7)。在其父亲的血液DNA中未检测到该缺失,我们强烈怀疑这是NF2的一种嵌合形式。
眼科表现可能是儿童NF2的初始症状。对于有NF2风险的个体,在生命的第一年必须积极寻找这些特征。NF2嵌合体通常被描述为NF2的一种轻度形式,向携带者子女的传播风险非常低。我们表明,NF2嵌合体有时会发展为严重的NF2症状,并且我们证实向后代的传播风险取决于携带突变的合子比例。NF2仍然是一种危及生命和影响生活质量的疾病。早期诊断对于预防并发症是必要的,并且NF2患者的随访必须在专业中心进行终身安排。
