A molecular, clinical, and immunohistochemical study of vestibular schwannoma

The molecular pathogenesis of vestibular schwannoma has been investigated by determining the extent of chromosome 22 loss of heterozygosity in 77 tumors and relating these findings to clinical and immunohistochemical indexes of tumor behavior. Loss of heterozygosity was looked for at eight chromosom...

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Published inOtolaryngology-head and neck surgery Vol. 116; no. 4; p. 426
Main Authors Irving, R M, Moffat, D A, Hardy, D G, Barton, D E, Xuereb, J H, Holland, F J, Maher, E R
Format Journal Article
LanguageEnglish
Published England 01.04.1997
Subjects
Adult
Aged
Alleles
Antibodies, Monoclonal
Cell Division
Chromosome Deletion
Chromosome Mapping
Chromosomes, Human, Pair 22 - genetics
Ear Neoplasms - genetics
Ear Neoplasms - pathology
Female
Gene Expression Regulation, Neoplastic - genetics
Genes, Neurofibromatosis 2 - genetics
Heterozygote
Humans
Immunohistochemistry
Male
Microsatellite Repeats - genetics
Middle Aged
Molecular Biology
Mutation - genetics
Neuroma, Acoustic - genetics
Neuroma, Acoustic - pathology
Proliferating Cell Nuclear Antigen - analysis
Vestibular Diseases - genetics
Vestibular Diseases - pathology
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Summary:The molecular pathogenesis of vestibular schwannoma has been investigated by determining the extent of chromosome 22 loss of heterozygosity in 77 tumors and relating these findings to clinical and immunohistochemical indexes of tumor behavior. Loss of heterozygosity was looked for at eight chromosome 22q loci. Clinical details were obtained in all 77 cases, and a clinical growth index was calculated for each tumor. The proliferative index was estimated in all tumors by using a monoclonal antibody to the proliferating cell nuclear antigen and by calculating the labeling index. Forty percent (31 of 77) of the tumors showed allele loss, and in each case this loss involved the region of the neurofibromatosis type 2 gene. No evidence was found that the presence of chromosome 22 allele loss was associated with the clinical growth index. On the log scale, however, an association was seen between the clinical growth index and the proliferating cell nuclear antigen labeling index p = 0.001). These results suggest that chromsome 22 allele loss is a frequent event in vestibular schwannoma. Tumor behavior, however, appears to be independent of the chromosome 22 mutation. It is proposed that chromosome 22 allele loss and neurofibromatosis type 2 gene inactivation is an early event, possibly involved in the initiation of tumorigenesis in vestibular schwannoma. Tumor growth appears to be independent of this mutation and is likely to be determined by other as yet undefined factors.
ISSN:0194-5998
1097-6817
DOI:10.1016/S0194-59989770289-4