BMC Genomics (Oct 2007)

Large-scale analysis by SAGE reveals new mechanisms of <it>v-erbA </it>oncogene action

  • Faure Claudine,
  • Keime Celine,
  • Bresson Corinne,
  • Letrillard Yann,
  • Barbado Maud,
  • Sanfilippo Sandra,
  • Benhra Najate,
  • Gandrillon Olivier,
  • Gonin-Giraud Sandrine

DOI
https://doi.org/10.1186/1471-2164-8-390
Journal volume & issue
Vol. 8, no. 1
p. 390

Abstract

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Abstract Background: The v-erbA oncogene, carried by the Avian Erythroblastosis Virus, derives from the c-erbAα proto-oncogene that encodes the nuclear receptor for triiodothyronine (T3R). v-ErbA transforms erythroid progenitors in vitro by blocking their differentiation, supposedly by interference with T3R and RAR (Retinoic Acid Receptor). However, v-ErbA target genes involved in its transforming activity still remain to be identified. Results: By using Serial Analysis of Gene Expression (SAGE), we identified 110 genes deregulated by v-ErbA and potentially implicated in the transformation process. Bioinformatic analysis of promoter sequence and transcriptional assays point out a potential role of c-Myb in the v-ErbA effect. Furthermore, grouping of newly identified target genes by function revealed both expected (chromatin/transcription) and unexpected (protein metabolism) functions potentially deregulated by v-ErbA. We then focused our study on 15 of the new v-ErbA target genes and demonstrated by real time PCR that in majority their expression was activated neither by T3, nor RA, nor during differentiation. This was unexpected based upon the previously known role of v-ErbA. Conclusion: This paper suggests the involvement of a wealth of new unanticipated mechanisms of v-ErbA action.