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Molecular Pathology 2003;56:299-301; doi:10.1136/mp.56.5.299
Copyright © 2003 by the BMJ Publishing Group Ltd & Association of Clinical Pathologists.
Molecular Pathology 2003;56:299-301
© 2003 BMJ Publishing Group Ltd. & Association of Clinical Pathologists

SHORT REPORT

Molecular heterogeneity of meningioma with INI1 mutation

P Rieske1, M Zakrzewska1, S Piaskowski1, D Jaskólski2, B Sikorska1, W Papierz3, K Zakrzewski4, P P Liberski1

1 Department of Molecular Pathology and Neurology, Medical University, 92–216 Lodz, Poland
2 Department of Neurosurgery, Medical University
3 Department of Pathomorphology, Medical University
4 Department of Neurosurgery, Polish Mother’s Memorial Hospital, 93–338 Lodz, Poland

Correspondence to:
Correspondence to:
Dr P Rieske, Department of Molecular Pathology and Neuropathology, Medical University Lodz, Czechoslowacka st.8/10, 92–216 Lodz, Poland;
Rieske{at}excite.com

ABSTRACT

Background: INI1 (hSNF5) mutations are linked to rhabdoid tumours, but mutations in meningiomas with hot spot mutations in position 377 have also been reported.

Aims: To analyse the INI1 gene in meningioma.

Methods: Exons 1, 4, 5, and 9 of the INI1 gene were analysed by the polymerase chain reaction and direct sequencing in 80 meningiomas. For all cases, western blotting of the INI1 protein was performed.

Results: Only one of the 80 samples showed a cytosine insertion in codon 376. This mutation changed the open reading frame in almost the whole exon 9 and resulted in a longer hSNF5 protein. Complex analysis of the above described tumour sample by western blotting, DNA sequencing, and loss of heterozygosity (LOH) analysis showed that this particular meningioma consisted of heterogeneic cellular components. One of these components had a mutated INI1 gene, whereas in the other component INI1 was intact.

Conclusions: INI1 mutation is a rare event in the molecular pathology of meningiomas. It is possible for the INI1 gene to be mutated in only a proportion of meningioma cells.

Keywords: loss of heterozygosity; meningioma; molecular heterogeneity; INI1; hSNF5

Abbreviations: LOH, loss of heterozygosity; NES, nuclear export signal; NF2, neurofibromin 2; INI1, integrase interactor 1; PCR, polymerase chain reaction


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