Literature DB >> 21325297

A multilocus technique for risk evaluation of patients with neuroblastoma.

Inge M Ambros1, Bettina Brunner, Gerhard Aigner, Clare Bedwell, Klaus Beiske, Jean Bénard, Nick Bown, Valerie Combaret, Jerome Couturier, Raffaella Defferrari, Nicole Gross, Marta Jeison, John Lunec, Barbara Marques, Tommy Martinsson, Katia Mazzocco, Rosa Noguera, Gudrun Schleiermacher, Frank Speleman, Ray Stallings, Gian Paolo Tonini, Deborah A Tweddle, Alexander Valent, Ales Vicha, Nadine Van Roy, Eva Villamon, Andrea Ziegler, Sandra Preuner, Mario Drobics, Ruth Ladenstein, Gabriele Amann, Robert J L Schuit, Ulrike Pötschger, Peter F Ambros.   

Abstract

PURPOSE: Precise and comprehensive analysis of neuroblastoma genetics is essential for accurate risk evaluation and only pangenomic/multilocus approaches fulfill the present-day requirements. We present the establishment and validation of the PCR-based multiplex ligation-dependent probe amplification (MLPA) technique for neuroblastoma. EXPERIMENTAL
DESIGN: A neuroblastoma-specific MLPA kit was designed by the SIOP Europe Neuroblastoma Biology Committee in cooperation with MRC-Holland. The contained target sequences cover 19 chromosomal arms and reference loci. Validation was performed by single locus and pangenomic techniques (n = 174). Dilution experiments for determination of minimal tumor cell percentage were performed and testing of reproducibility was checked by interlaboratory testing (n = 15). Further 156 neuroblastomas were used for establishing the amplification cutoff level.
RESULTS: The MLPA technique was tested in 310 neuroblastomas and 8 neuroblastoma cell lines (including validation and amplification cutoff level testing). Intertechnique validation showed a high concordance rate (99.5%). Interlaboratory MLPA testing (κ = 0.95, P < 0.01) revealed 7 discrepant of 1,490 results (0.5%). Validation by pangenomic techniques showed a single discordance of 190 consensus results (0.5%). The test results led to formulation of interpretation standards and to a kit revision. The minimal tumor cell percentage was fixed at 60%.
CONCLUSIONS: The recently designed neuroblastoma-specific MLPA kit covers all chromosomal regions demanded by the International Neuroblastoma Risk Group for therapy stratification and includes all hitherto described genetic loci of prognostic interest for future studies and can be modified or extended at any time. Moreover, the technique is cost effective, reliable, and robust with a high interlaboratory and intertechnique concordance. ©2011 AACR.

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Year:  2011        PMID: 21325297     DOI: 10.1158/1078-0432.CCR-10-0830

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  12 in total

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Journal:  Neoplasia       Date:  2012-09       Impact factor: 5.715

2.  Comparative genetic study of intratumoral heterogenous MYCN amplified neuroblastoma versus aggressive genetic profile neuroblastic tumors.

Authors:  A P Berbegall; E Villamón; M Piqueras; I Tadeo; A Djos; P F Ambros; T Martinsson; I M Ambros; A Cañete; V Castel; S Navarro; R Noguera
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3.  Investigation of major genetic alterations in neuroblastoma.

Authors:  Régis Afonso Costa; Héctor N Seuánez
Journal:  Mol Biol Rep       Date:  2018-02-17       Impact factor: 2.316

4.  Expression of miR-487b and miR-410 encoded by 14q32.31 locus is a prognostic marker in neuroblastoma.

Authors:  C-H Gattolliat; L Thomas; S A Ciafrè; G Meurice; G Le Teuff; B Job; C Richon; V Combaret; P Dessen; D Valteau-Couanet; E May; P Busson; S Douc-Rasy; J Bénard
Journal:  Br J Cancer       Date:  2011-10-04       Impact factor: 7.640

5.  How to minimise the effect of tumour cell content in detection of aberrant genetic markers in neuroblastoma.

Authors:  M Piqueras; S Navarro; A Cañete; V Castel; R Noguera
Journal:  Br J Cancer       Date:  2011-06-07       Impact factor: 7.640

6.  Segmental chromosomal alterations lead to a higher risk of relapse in infants with MYCN-non-amplified localised unresectable/disseminated neuroblastoma (a SIOPEN collaborative study).

Authors:  G Schleiermacher; J Michon; A Ribeiro; G Pierron; V Mosseri; H Rubie; C Munzer; J Bénard; N Auger; V Combaret; I Janoueix-Lerosey; A Pearson; D A Tweddle; N Bown; M Gerrard; K Wheeler; R Noguera; E Villamon; A Cañete; V Castel; B Marques; A de Lacerda; G P Tonini; K Mazzocco; R Defferrari; B de Bernardi; A di Cataldo; N van Roy; B Brichard; R Ladenstein; I Ambros; P Ambros; K Beiske; O Delattre; J Couturier
Journal:  Br J Cancer       Date:  2011-11-10       Impact factor: 7.640

7.  Genetic instability and intratumoral heterogeneity in neuroblastoma with MYCN amplification plus 11q deletion.

Authors:  Eva Villamón; Ana P Berbegall; Marta Piqueras; Irene Tadeo; Victoria Castel; Anna Djos; Tommy Martinsson; Samuel Navarro; Rosa Noguera
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8.  Frequency and Prognostic Impact of ALK Amplifications and Mutations in the European Neuroblastoma Study Group (SIOPEN) High-Risk Neuroblastoma Trial (HR-NBL1).

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9.  Neuroblastoma after childhood: prognostic relevance of segmental chromosome aberrations, ATRX protein status, and immune cell infiltration.

Authors:  Ana P Berbegall; Eva Villamón; Irene Tadeo; Tommy Martinsson; Adela Cañete; Victoria Castel; Samuel Navarro; Rosa Noguera
Journal:  Neoplasia       Date:  2014-06       Impact factor: 5.715

10.  Expression of two parental imprinted miRNAs improves the risk stratification of neuroblastoma patients.

Authors:  Charles-Henry Gattolliat; Gwénaël Le Teuff; Valérie Combaret; Eugénie Mussard; Dominique Valteau-Couanet; Pierre Busson; Jean Bénard; Sétha Douc-Rasy
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