Skip to main content
Article
Senescence-Associated Gene YPEL3 Is Downregulated in Human Colon Tumors
Annals of Surgical Oncology
  • Rebecca Tuttle, Wright State University
  • Margo Simon, Wright State University
  • David C. Hitch, Wright State University
  • J. Nicholas Maiorano, Wright State University
  • Minia Hellan, Wright State University
  • James R. Ouellette, Wright State University
  • Paula M. Termuhlen, Wright State University
  • Steven J. Berberich, Wright State University - Main Campus
Document Type
Article
Publication Date
6-1-2011
Abstract

Background

Previous work has demonstrated YPEL3 to be a growth-suppressive protein that acts through a pathway of cellular senescence. We set out to determine whether human colon tumors demonstrated downregulation of YPEL3. Methods

We collected colon tumor samples with matched normal control samples and analyzed them forYPEL3 gene expression by reverse transcriptase–polymerase chain reaction and CpG hypermethylation of the YPEL3 promoter by base-specific polymerase chain reaction analysis. Colon cancer cell lines (Caco-2 and HCT116−/− p53) were used to assess YPEL3 gene expression after treatment with 5-azadeoxycytidine or trichostatin A. Results

Reverse transcriptase–polymerase chain reaction analysis demonstrated a decrease in YPEL3expression in tumor samples when compared to their patient-matched normal tissue. We determined that DNA methylation of the YPEL3 promoter CpG island does not play a role in YPEL3 regulation in human colon tumors or colon cancer cells lines, consistent with the inability of 5-azadeoxycytidine treatment to induce YPEL3 expression in colon cancer cell lines. In contrast, colon cell line results suggest that histone acetylation may play a role in YPEL3 regulation in colon cancer. Conclusions

YPEL3 is preferentially downregulated in human colon adenocarcinomas. DNA hypermethylation does not appear to be the mechanism of YPEL3 downregulation in this subset of collected patient samples or in colon cell lines. Histone acetylation may be a relevant epigenetic modulator of YPEL3in colon adenocarcinomas. Future investigation of YPEL3 and its role in colon cancer signaling and development may lead to increased understanding and alternative treatment options for this disease.

DOI
10.1245/s10434-011-1558-x
Citation Information
Rebecca Tuttle, Margo Simon, David C. Hitch, J. Nicholas Maiorano, et al.. "Senescence-Associated Gene YPEL3 Is Downregulated in Human Colon Tumors" Annals of Surgical Oncology Vol. 18 Iss. 6 (2011) p. 1791 - 1796 ISSN: 10689265
Available at: http://works.bepress.com/rebecca_tuttle/5/