BMC Genomics (May 2008)

Global analysis of aberrant pre-mRNA splicing in glioblastoma using exon expression arrays

  • Nixon Tamara J,
  • Neubauer Valerie L,
  • Bachinski Linda L,
  • Tsavachidis Spiridon,
  • Baggerly Keith A,
  • Cheung Hannah C,
  • Aldape Kenneth D,
  • Cote Gilbert J,
  • Krahe Ralf

DOI
https://doi.org/10.1186/1471-2164-9-216
Journal volume & issue
Vol. 9, no. 1
p. 216

Abstract

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Abstract Background Tumor-predominant splice isoforms were identified during comparative in silico sequence analysis of EST clones, suggesting that global aberrant alternative pre-mRNA splicing may be an epigenetic phenomenon in cancer. We used an exon expression array to perform an objective, genome-wide survey of glioma-specific splicing in 24 GBM and 12 nontumor brain samples. Validation studies were performed using RT-PCR on glioma cell lines, patient tumor and nontumor brain samples. Results In total, we confirmed 14 genes with glioma-specific splicing; seven were novel events identified by the exon expression array (A2BP1, BCAS1, CACNA1G, CLTA, KCNC2, SNCB, and TPD52L2). Our data indicate that large changes (> 5-fold) in alternative splicing are infrequent in gliomagenesis ( Conclusion While we observed some tumor-specific alternative splicing, the number of genes showing exclusive tumor-specific isoforms was on the order of tens, rather than the hundreds suggested previously by in silico mining. Given the important role of alternative splicing in neural differentiation, there may be selective pressure to maintain a majority of splicing events in order to retain glial-like characteristics of the tumor cells.