| Literature DB >> 30993672 |
Dorothy Halliday1,2, Beatrice Emmanouil2,3, Grace Vassallo4, Karine Lascelles5, James Nicholson6, Saleel Chandratre7, Geetha Anand8, Martin Wasik9, Pieter Pretorius10, D Gareth Evans11, Allyson Parry2,12.
Abstract
Childhood onset neurofibromatosis type 2 can be severe and genotype dependent. We present a retrospective phenotypic analysis of all ascertained children in England <age 18 (N = 87; male 61%). Mean age at last review was 13.9 years with mean follow-up 6.5 years. Patients were stratified using a validated score (1A/1B:no NF2 pathogenic_variant in blood; 2A/2B:mild/moderate NF2 constitutional or mosaic pathogenic_variant in blood; 3: constitutional truncating exon 2-13 pathogenic_variant. A total of 91% patients had a constitutional NF2 pathogenic_variant (44% de novo). Mean age at first manifestation was 4.3 and 8.8 years in groups 3 and 2A, respectively. Bilateral vestibular schwannoma, intracranial meningioma and spinal schwannoma occurred in 77%, 52% and 65% of group 3 patients, respectively, and 58%, 26% and 33% in 2A. A total of 43% group 3 and 18% 2A had severe unilateral visual loss (logmar >1.0). Focal cortical dysplasia occurred in 26% group 3 and 4% 2A. A total of 48% of group 3 underwent ≥1 major intervention (intracranial/spinal surgery/Bevacizumab/radiotherapy) compared to 35% of 2A; with 23% group 3 undergoing spinal surgery (schwannoma/ependymoma/meningioma resection) compared to 4% of 2A. Mean age starting Bevacizumab was 12.7 in group 3 and 14.9 years in 2A. In conclusion, group 3 phenotype manifests earlier with greater tumour load, poorer visual outcomes and more intervention.Entities:
Keywords: NF2; NF2 genetic severity score; childhood NF2; paediatric NF2 genotype phenotype
Year: 2019 PMID: 30993672 DOI: 10.1111/cge.13551
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438