TY - JOUR
T1 - Clinical and molecular predictors of mortality in neurofibromatosis 2
T2 - A UK national analysis of 1192 patients
AU - The English Specialist NF2 Research Group
AU - Hexter, Adam
AU - Jones, Adrian
AU - Joe, Harry
AU - Heap, Laura
AU - Smith, Miriam J.
AU - Wallace, Andrew J.
AU - Halliday, Dorothy
AU - Parry, Allyson
AU - Taylor, Amy
AU - Raymond, Lucy
AU - Shaw, Adam
AU - Afridi, Shazia
AU - Obholzer, Rupert
AU - Axon, Patrick
AU - King, Andrew T.
AU - Friedman, Jan M.
AU - D Gareth R, Gareth R
AU - Burnet, Neil
AU - Donnelly, Neil
AU - Durie-Gair, Juliette
AU - English, Martin
AU - Folland, Nicola
AU - Foweraker, Karen
AU - Harris, Fiona
AU - Harris, Frances
AU - Heney, David
AU - Jeffries, Sarah
AU - Jena, Raj
AU - Knight, Richard
AU - Lamb, Tamara
AU - Macfarlane, Robert
AU - Mannion, Richard
AU - Nicholson, James
AU - Price, Richard
AU - Rands, Ella
AU - Sanghera, Paul
AU - Scoffings, Daniel
AU - Tysome, James
AU - Ferner, Rosalie E.
AU - Hammond, Chris
AU - Lascelles, Karine
AU - Nunn, Terry
AU - Saeed, Shakeel
AU - Swampillai, Angela
AU - Thomson, Suki
AU - Walsh, Daniel
AU - Williams, Victoria
AU - Dalton, Louise
AU - Hanemann, C. Oliver
AU - Kerr, Richard
PY - 2015/8/14
Y1 - 2015/8/14
N2 - Background Neurofibromatosis 2 (NF2) is an autosomal-dominant tumour predisposition syndrome characterised by bilateral vestibular schwannomas, considerable morbidity and reduced life expectancy. Although genotype-phenotype correlations are well established in NF2, little is known about effects of mutation type or location within the gene on mortality. Improvements in NF2 diagnosis and management have occurred, but their effect on patient survival is unknown. Methods We evaluated clinical and molecular predictors of mortality in 1192 patients (771 with known causal mutations) identified through the UK National NF2 Registry. Kaplan-Meier survival and Cox regression analyses were used to evaluate predictors of mortality, with jackknife adjustment of parameter SEs to account for the strong intrafamilial phenotypic correlations that occur in NF2. Results The study included 241 deaths during 10 995 patient-years of follow-up since diagnosis. Early age at diagnosis and the presence of intracranial meningiomas were associated with increased mortality, and having a mosaic, rather than non-mosaic, NF2 mutation was associated with reduced mortality. Patients with splicesite or missense mutations had lower mortality than patients with truncating mutations (OR 0.459, 95% CI 0.213 to 0.990, and OR 0.196, 95% CI 0.213 to 0.990, respectively). Patients with splice-site mutations in exons 6-15 had lower mortality than patients with splice-site mutations in exons 1-5 (OR 0.333, 95% CI 0.129 to 0.858). The mortality of patients with NF2 diagnosed in more recent decades was lower than that of patients diagnosed earlier. Conclusions Continuing advances in molecular diagnosis, imaging and treatment of NF2-associated tumours offer hope for even better survival in the future.
AB - Background Neurofibromatosis 2 (NF2) is an autosomal-dominant tumour predisposition syndrome characterised by bilateral vestibular schwannomas, considerable morbidity and reduced life expectancy. Although genotype-phenotype correlations are well established in NF2, little is known about effects of mutation type or location within the gene on mortality. Improvements in NF2 diagnosis and management have occurred, but their effect on patient survival is unknown. Methods We evaluated clinical and molecular predictors of mortality in 1192 patients (771 with known causal mutations) identified through the UK National NF2 Registry. Kaplan-Meier survival and Cox regression analyses were used to evaluate predictors of mortality, with jackknife adjustment of parameter SEs to account for the strong intrafamilial phenotypic correlations that occur in NF2. Results The study included 241 deaths during 10 995 patient-years of follow-up since diagnosis. Early age at diagnosis and the presence of intracranial meningiomas were associated with increased mortality, and having a mosaic, rather than non-mosaic, NF2 mutation was associated with reduced mortality. Patients with splicesite or missense mutations had lower mortality than patients with truncating mutations (OR 0.459, 95% CI 0.213 to 0.990, and OR 0.196, 95% CI 0.213 to 0.990, respectively). Patients with splice-site mutations in exons 6-15 had lower mortality than patients with splice-site mutations in exons 1-5 (OR 0.333, 95% CI 0.129 to 0.858). The mortality of patients with NF2 diagnosed in more recent decades was lower than that of patients diagnosed earlier. Conclusions Continuing advances in molecular diagnosis, imaging and treatment of NF2-associated tumours offer hope for even better survival in the future.
UR - http://www.scopus.com/inward/record.url?scp=84946477803&partnerID=8YFLogxK
U2 - 10.1136/jmedgenet-2015-103290
DO - 10.1136/jmedgenet-2015-103290
M3 - Article
C2 - 26275417
AN - SCOPUS:84946477803
SN - 0022-2593
VL - 52
SP - 699
EP - 705
JO - Journal of Medical Genetics
JF - Journal of Medical Genetics
IS - 10
ER -