Journal
MOLECULAR ONCOLOGY
Volume 7, Issue 3, Pages 419-427Publisher
WILEY
DOI: 10.1016/j.molonc.2012.11.005
Keywords
SALL2; Ovarian cancer; Tumor suppressor; Promoter methylation; Polyoma T antigen
Categories
Funding
- National Cancer Institute [RO1 CA-092520]
- Ovarian Cancer Research Fund
- Mary Kay Foundation
- Robert and Debra First Fund
- Dana-Farber Women's Executive Council Genetic Fingerprinting Award
- [P50 CA105009]
- [U01 CA152990]
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The SALL2 gene product and transcription factor p150 were first identified in a search for tumor suppressors targeted for inactivation by the oncogenic mouse polyoma virus. SALL2 has also been identified as a cellular quiescence factor, essential for cells to enter and remain in a state of growth arrest under conditions of serum deprivation. p150 is a transcriptional activator of p21(Cip1/Waf1) and BAX, sharing important growth arrest and proapoptotic properties with p53. It also acts as a repressor of c-myc. Restoration of SALL2 expression in cells derived from a human ovarian carcinoma (OVCA) suppresses growth of the cells in immunodeficient mice. Here we examine the pattern of p150 expression in the normal human ovary, in OVCA-derived cell lines and in primary ovarian carcinomas. Immunohistochemical staining showed that p150 is highly expressed in surface epithelial cells of the normal human ovary. Expression is exclusively from the P2 promoter governing the E1A splice variant of p150. The P2 promoter is CpG-rich and susceptible to methylation silencing. p150 expression was restored in OVCA cell lines following growth in the presence of 5-azacytidine. In a survey of 210 cases of OVCA, roughly 90% across major and minor histological types failed to show expression of the protein. Immunological and biochemical approaches were used to show hypermethylation of the SALL2 P2 promoter in OVCA-derived cell lines and in a majority of primary tumors. These results bring together molecular biological and clinical evidence in support of a role of SALL2 as a suppressor of ovarian cancers. (C) 2012 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.
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