Literature DB >> 15494096

Diagnostic and prognostic significance of genetic regional heterogeneity in meningiomas.

Wolfgang K Pfisterer1, Nicole C Hank, Mark C Preul, William P Hendricks, Jeanette Pueschel, Stephen W Coons, Adrienne C Scheck.   

Abstract

We analyzed the frequency and regional distribution of cells with genetic abnormalities of chromosomes 1, 14, and 22 in meningiomas. This data was evaluated for correlation to the clinical outcome of the patients. Eight defined areas of each of 77 paraffin-embedded meningioma samples (59 grade I, 13 grade II, and 5 grade III) were analyzed by fluorescent in situ hybridization using bacterial artificial chromosome probes localized to chromosomes 1p36.32, 1q25.3, 14q13.3, 14q32.12, 22q11.2, and 22q12.1-3. Chromosome deletion was considered to be regionally heterogeneous if 7 regions showed cells with chromosome deletions. Deletion of 1p occurred in 35% of the grade I tumors. Distribution of cells with 1p deletion was regionally heterogeneous in 25% and homogeneous in 10% of grade I tumors. Distribution of cells with deletion of 1p was regionally heterogeneous in 23% and homogeneous in 69% of the grade II tumors. All grade III meningiomas had homogeneous distribution of cells with deletion of chromosome 1p. Distribution of cells with deletion of 14q was regionally heterogeneous in 27% and homogeneous in 2% of the grade I meningiomas, heterogeneous in 31% and homogeneous in 62% of the grade II tumors, and heterogeneous in 40% and homogeneous in 60% of the grade III meningiomas. Distribution of cells with deletion of 22q was regionally heterogeneous in 15% and homogeneous in 3% of the grade I tumors, heterogeneous in 15% and homogeneous in 31% of grade II tumors, and homogeneous in 20% of the grade III meningiomas. Distribution of cells with trisomy 22q was regionally heterogeneous in 10% of grade I tumors, heterogeneous in 23% of grade II, and homogeneous in 80% of grade III meningiomas. The proportion of patients with a deletion of 22q (either homogeneous or heterogeneous) who had recurrence was greater than the proportion of those without 22q deletion who had recurrence, and deletion of 22q was significantly associated with radiologically detected recurrence (P < 0.05). We conclude that the appearance of chromosomal aberrations in different areas of the tumor demonstrates the importance of regional heterogeneity in the biological behavior of meningiomas.

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Year:  2004        PMID: 15494096      PMCID: PMC1872008          DOI: 10.1215/S1152851704000158

Source DB:  PubMed          Journal:  Neuro Oncol        ISSN: 1522-8517            Impact factor:   12.300


  48 in total

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2.  The recurrence of intracranial meningiomas after surgical treatment.

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3.  Gains of chromosome 22 by fluorescence in situ hybridization in the context of an hyperdiploid karyotype are associated with aggressive clinical features in meningioma patients.

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4.  Chromosome 1p and 14q FISH analysis in clinicopathologic subsets of meningioma: diagnostic and prognostic implications.

Authors:  D X Cai; R Banerjee; B W Scheithauer; C M Lohse; B K Kleinschmidt-Demasters; A Perry
Journal:  J Neuropathol Exp Neurol       Date:  2001-06       Impact factor: 3.685

5.  Telomerase activity and expression of the telomerase catalytic subunit, hTERT, in meningioma progression.

Authors:  M Simon; T W Park; S Leuenroth; V H Hans; T Löning; J Schramm
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6.  Analysis of p73 gene in meningiomas with deletion at 1p.

Authors:  J Lomas; M J Bello; D Arjona; P Gonzalez-Gomez; M E Alonso; J M de Campos; J Vaquero; P Ruiz-Barnes; J L Sarasa; C Casartelli; J A Rey
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7.  Loss of 1p in recurrent meningiomas. a comparative study in successive recurrences by cytogenetics and fluorescence in situ hybridization.

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8.  High-resolution analysis of chromosome arm 1p alterations in meningioma.

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Journal:  Cancer Genet Cytogenet       Date:  2000-07-01

9.  Alterations of INK4a(p16-p14ARF)/INK4b(p15) expression and telomerase activation in meningioma progression.

Authors:  M Simon; T W Park; G Köster; R Mahlberg; M Hackenbroch; J Boström; T Löning; J Schramm
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10.  Tight association of loss of merlin expression with loss of heterozygosity at chromosome 22q in sporadic meningiomas.

Authors:  K Ueki; C Wen-Bin; Y Narita; A Asai; T Kirino
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  12 in total

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2.  1p36.32 rearrangements and the role of PI-PLC η2 in nervous tumours.

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3.  Intratumor and informatic heterogeneity influence meningioma molecular classification.

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4.  Monosomy of chromosome 10 associated with dysregulation of epidermal growth factor signaling in glioblastomas.

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5.  Implicating chromosomal aberrations with meningioma growth and recurrence: results from FISH and MIB-I analysis of grades I and II meningioma tissue.

Authors:  Wolfgang K Pfisterer; Stephen W Coons; Fahmy Aboul-Enein; William P Hendricks; Adrienne C Scheck; Mark C Preul
Journal:  J Neurooncol       Date:  2007-11-30       Impact factor: 4.130

6.  Proposal for a new risk stratification classification for meningioma based on patient age, WHO tumor grade, size, localization, and karyotype.

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7.  Proteins involved in regulating bone invasion in skull base meningiomas.

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Journal:  Acta Neurochir (Wien)       Date:  2012-12-13       Impact factor: 2.216

Review 8.  The current status of 5-ALA fluorescence-guided resection of intracranial meningiomas-a critical review.

Authors:  Arash Motekallemi; Hanne-Rinck Jeltema; Jan D M Metzemaekers; Gooitzen M van Dam; Lucy M A Crane; Rob J M Groen
Journal:  Neurosurg Rev       Date:  2015-03-05       Impact factor: 3.042

9.  Nanofiber-mediated inhibition of focal adhesion kinase sensitizes glioma stemlike cells to epidermal growth factor receptor inhibition.

Authors:  Maya Srikanth; Sunit Das; Eric J Berns; Juno Kim; Samuel I Stupp; John A Kessler
Journal:  Neuro Oncol       Date:  2013-01-17       Impact factor: 12.300

10.  Gene expression profiles of metabolic aggressiveness and tumor recurrence in benign meningioma.

Authors:  Eva Serna; José Manuel Morales; Manuel Mata; José Gonzalez-Darder; Teresa San Miguel; Rosario Gil-Benso; Concha Lopez-Gines; Miguel Cerda-Nicolas; Daniel Monleon
Journal:  PLoS One       Date:  2013-06-28       Impact factor: 3.240

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