Literature DB >> 22278416

Epigenetic and copy number variation analysis in retinoblastoma by MS-MLPA.

Gabriella Livide1, Maria Carmela Epistolato, Mariangela Amenduni, Vittoria Disciglio, Annabella Marozza, Maria Antonietta Mencarelli, Paolo Toti, Stefano Lazzi, Theodora Hadjistilianou, Sonia De Francesco, Alfonso D'Ambrosio, Alessandra Renieri, Francesca Ariani.   

Abstract

Retinoblastoma is the most common primary intraocular malignancy in children. Two step inactivation of RB1 (M1-M2) represents the key event in the pathogenesis of retinoblastoma but additional genetic and epigenetic events (M3-Mn) are required for tumor development. In the present study, we employed Methylation Specific Multiplex Ligation Probe Assay to investigate methylation status and copy number changes of 25 and 39 oncosuppressor genes, respectively. This technique was applied to analyse 12 retinoblastomas (5 bilateral and 7 unilateral) and results were compared to corresponding normal retina. We identified hypermethylation in seven new genes: MSH6 (50%), CD44 (42%), PAX5 (42%), GATA5 (25%), TP53 (8%), VHL (8%) and GSTP1 (8%) and we confirmed the previously reported hypermethylation of MGMT (58%), RB1 (17%) and CDKN2 (8%). These genes belong to key pathways including DNA repair, pRB and p53 signalling, transcriptional regulation, protein degradation, cell-cell interaction, cellular adhesion and migration. In the same group of retinoblastomas, a total of 29 copy number changes (19 duplications and 10 deletions) have been identified. Interestingly, we found deletions of the following oncosuppressor genes that might contribute to drive retinoblastoma tumorigenesis: TP53, CDH13, GATA5, CHFR, TP73 and IGSF4. The present data highlight the importance of epigenetic changes in retinoblastoma and indicate seven hypermethylated oncosuppressors never associated before to retinoblastoma pathogenesis. This study also confirms the presence of copy number variations in retinoblastoma, expecially in unilateral cases (mean 3 ± 1.3) where these changes were found more frequently respect to bilateral cases (mean 1.4 ± 1.1).

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Year:  2012        PMID: 22278416     DOI: 10.1007/s12253-012-9498-8

Source DB:  PubMed          Journal:  Pathol Oncol Res        ISSN: 1219-4956            Impact factor:   3.201


  83 in total

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Journal:  Cancer Res       Date:  2001-02-15       Impact factor: 12.701

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5.  Impaired expression and promotor hypermethylation of O6-methylguanine-DNA methyltransferase in retinoblastoma tissues.

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  24 in total

Review 1.  Epigenetic regulation of human retinoblastoma.

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Review 4.  A Tox21 Approach to Altered Epigenetic Landscapes: Assessing Epigenetic Toxicity Pathways Leading to Altered Gene Expression and Oncogenic Transformation In Vitro.

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Review 5.  The genomic landscape of retinoblastoma: a review.

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Review 8.  Biomarkers in retinoblastoma.

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9.  Epigenetics in ocular diseases.

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10.  More epigenetic hits than meets the eye: microRNAs and genes associated with the tumorigenesis of retinoblastoma.

Authors:  Adriana H O Reis; Fernando R Vargas; Bernardo Lemos
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