The Ewing's family of tumors (EFTs) are characterized by chimeric transcripts generated by specific chromosomal rearrangements. The most common fusions are between the EWSR1 gene on chromosome 22 and the ETS family of transcription factors; rarely, FUS (on chromosome 16) substitutes for EWSR1. The detection of specific translocations using molecular analysis is now a routine part of the pathological examination of EFT. Here, we report our experience with molecular diagnosis of EFT during the 4 years (2006-2009) at the Rizzoli Institute. We analyzed 222 consecutive tumors with a presumptive diagnosis of EFT using molecular techniques and IHC. We found five distinct types of EWSR1-FLI1 fusion transcripts resulting from translocation t(11;22), three types of EWSR1-ERG transcripts resulting from t(21;22), and one type of t(2;22) resulting in EWSR1-FEV fusion. Molecular investigation validated 92% of cases ultimately diagnosed as EFT; IHC validated 76% of the cases. Thus, despite the difficulties and limitations associated with both molecular and IHC analysis on fresh and formalin-fixed, paraffin-embedded tissue, a combination of these techniques is the best approach to enhancing the accuracy of EFT diagnosis. We also present our method for choosing which molecular techniques to apply. Finally, we collected the most prevalent breakpoints reported in the literature, indicating which exons are involved, the sequence breakpoints, and the NCBI reference sequences.

Molecular diagnosis in ewing family tumors the rizzoli experience-222 consecutive cases in four years / Gamberi, Gabriella; Cocchi, Stefania; Benini, Stefania; Magagnoli, Giovanna; Morandi, Luca; Kreshak, Jennifer; Gambarotti, Marco; Picci, Piero; Zanella, Licciana; Alberghini, Marco. - In: THE JOURNAL OF MOLECULAR DIAGNOSTICS. - ISSN 1525-1578. - STAMPA. - 13:3(2011), pp. 313-324. [10.1016/j.jmoldx.2011.01.004]

Molecular diagnosis in ewing family tumors the rizzoli experience-222 consecutive cases in four years

GAMBERI, GABRIELLA;COCCHI, STEFANIA;MORANDI, LUCA;GAMBAROTTI, MARCO;PICCI, PIERO;ALBERGHINI, MARCO
2011

Abstract

The Ewing's family of tumors (EFTs) are characterized by chimeric transcripts generated by specific chromosomal rearrangements. The most common fusions are between the EWSR1 gene on chromosome 22 and the ETS family of transcription factors; rarely, FUS (on chromosome 16) substitutes for EWSR1. The detection of specific translocations using molecular analysis is now a routine part of the pathological examination of EFT. Here, we report our experience with molecular diagnosis of EFT during the 4 years (2006-2009) at the Rizzoli Institute. We analyzed 222 consecutive tumors with a presumptive diagnosis of EFT using molecular techniques and IHC. We found five distinct types of EWSR1-FLI1 fusion transcripts resulting from translocation t(11;22), three types of EWSR1-ERG transcripts resulting from t(21;22), and one type of t(2;22) resulting in EWSR1-FEV fusion. Molecular investigation validated 92% of cases ultimately diagnosed as EFT; IHC validated 76% of the cases. Thus, despite the difficulties and limitations associated with both molecular and IHC analysis on fresh and formalin-fixed, paraffin-embedded tissue, a combination of these techniques is the best approach to enhancing the accuracy of EFT diagnosis. We also present our method for choosing which molecular techniques to apply. Finally, we collected the most prevalent breakpoints reported in the literature, indicating which exons are involved, the sequence breakpoints, and the NCBI reference sequences.
2011
Molecular diagnosis in ewing family tumors the rizzoli experience-222 consecutive cases in four years / Gamberi, Gabriella; Cocchi, Stefania; Benini, Stefania; Magagnoli, Giovanna; Morandi, Luca; Kreshak, Jennifer; Gambarotti, Marco; Picci, Piero; Zanella, Licciana; Alberghini, Marco. - In: THE JOURNAL OF MOLECULAR DIAGNOSTICS. - ISSN 1525-1578. - STAMPA. - 13:3(2011), pp. 313-324. [10.1016/j.jmoldx.2011.01.004]
Gamberi, Gabriella; Cocchi, Stefania; Benini, Stefania; Magagnoli, Giovanna; Morandi, Luca; Kreshak, Jennifer; Gambarotti, Marco; Picci, Piero; Zanella, Licciana; Alberghini, Marco
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11585/529621
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