Burkitt lymphoma beyond MYC translocation: N-MYC and DNA methyltransferases dysregulation.

De Falco, Giulia; Ambrosio, Maria Raffaella; Fuligni, Fabio; Onnis, Anna; Bellan, Cristiana; Rocca, Bruno Jim; Navari, Mohsen; Etebari, Maryam; Mundo, Lucia; Gazaneo, Sara; Facchetti, Fabio; Pileri, Stefano A; Leoncini, Lorenzo; Piccaluga, Pier Paolo

De Falco, Giulia; Ambrosio, Maria Raffaella; Fuligni, Fabio; Onnis, Anna; Bellan, Cristiana; Rocca, Bruno Jim; Navari, Mohsen; Etebari, Maryam; Mundo, Lucia; Gazaneo, Sara; Facchetti, Fabio; Pileri, Stefano A; Leoncini, Lorenzo; Piccaluga, Pier Paolo.

Afiliación

De Falco G; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. defalco@unisi.it.
Ambrosio MR; School of Biological and Chemical Sciences, Queen Mary University of London, London, UK. defalco@unisi.it.
Fuligni F; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. maradot@libero.it.
Onnis A; Department of Experimental, Diagnostic, and Specialty Medicine, University of Bologna, Via Zamboni, 33, 40126, Bologna, Italy. fabio.fuligni2@unibo.it.
Bellan C; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. onnis2@unisi.it.
Rocca BJ; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. bellan@unisi.it.
Navari M; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. brunojim@libero.it.
Etebari M; Department of Experimental, Diagnostic, and Specialty Medicine, University of Bologna, Via Zamboni, 33, 40126, Bologna, Italy. navari@unisi.it.
Mundo L; Department of Experimental, Diagnostic, and Specialty Medicine, University of Bologna, Via Zamboni, 33, 40126, Bologna, Italy. etebary@unibo.it.
Gazaneo S; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. mundol@hotmail.it.
Facchetti F; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. sara.gazaneo@gmail.com.
Pileri SA; Unit of Pathology, Brescia University, Piazza del Mercato, 15, Brescia, Italy. facchett@med.unibs.it.
Leoncini L; Department of Experimental, Diagnostic, and Specialty Medicine, University of Bologna, Via Zamboni, 33, 40126, Bologna, Italy. stefano.pileri@unibo.it.
Piccaluga PP; Department of Medical Biotechnologies, University of Siena, Italy - Via delle Scotte, 6 - 53100, Siena, Italy. leoncinil@unisi.it.

BMC Cancer ; 15: 668, 2015 Oct 09.

Article en En | MEDLINE | ID: mdl-26453442

ABSTRACT

ABSTRACT

BACKGROUND:

The oncogenic transcription factor MYC is pathologically activated in many human malignancies. A paradigm for MYC dysregulation is offered by Burkitt lymphoma, where chromosomal translocations leading to Immunoglobulin gene-MYC fusion are the crucial initiating oncogenic events. However, Burkitt lymphoma cases with no detectable MYC rearrangement but maintaining MYC expression have been identified and alternative mechanisms can be involved in MYC dysregulation in these cases.

METHODS:

We studied the microRNA profile of MYC translocation-positive and MYC translocation-negative Burkitt lymphoma cases in order to uncover possible differences at the molecular level. Data was validated at the mRNA and protein level by quantitative Real-Time polymerase chain reaction and immunohistochemistry, respectively.

RESULTS:

We identified four microRNAs differentially expressed between the two groups. The impact of these microRNAs on the expression of selected genes was then investigated. Interestingly, in MYC translocation-negative cases we found over-expression of DNA-methyl transferase family members, consistent to hypo-expression of the hsa-miR-29 family. This finding suggests an alternative way for the activation of lymphomagenesis in these cases, based on global changes in methylation landscape, aberrant DNA hypermethylation, lack of epigenetic control on transcription of targeted genes, and increase of genomic instability. In addition, we observed an over-expression of another MYC family gene member, MYCN that may therefore represent a cooperating mechanism of MYC in driving the malignant transformation in those cases lacking an identifiable MYC translocation but expressing the gene at the mRNA and protein levels.

CONCLUSIONS:

Collectively, our results showed that MYC translocation-positive and MYC translocation-negative Burkitt lymphoma cases are slightly different in terms of microRNA and gene expression. MYC translocation-negative Burkitt lymphoma, similarly to other aggressive B-cell non Hodgkin's lymphomas, may represent a model to understand the intricate molecular pathway responsible for MYC dysregulation in cancer.

Asunto(s)

Linfoma de Burkitt/genética; Metilasas de Modificación del ADN/genética; Regulación Neoplásica de la Expresión Génica; Genes myc; Translocación Genética; Linfoma de Burkitt/metabolismo; Análisis por Conglomerados; Metilación de ADN; Metilasas de Modificación del ADN/metabolismo; Amplificación de Genes; Perfilación de la Expresión Génica; Humanos; MicroARNs/genética; Familia de Multigenes; ARN Mensajero/genética; ARN Mensajero/metabolismo; Reproducibilidad de los Resultados; Transcriptoma

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Translocación Genética / Metilasas de Modificación del ADN / Regulación Neoplásica de la Expresión Génica / Genes myc / Linfoma de Burkitt Tipo de estudio: Prognostic_studies Límite: Humans Idioma: En Revista: BMC Cancer Asunto de la revista: NEOPLASIAS Año: 2015 Tipo del documento: Article País de afiliación: Italia

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