@article{86f5d8e4625f4432a88a1c6dfcd16012,
title = "Analysis of EphA2 expression and mutant p53 in ovarian carcinoma",
abstract = "The EphA2 tyrosine kinase receptor is frequently overexpressed in ovarian cancer and this feature is predictive of poor clinical outcome. Preclinical investigation has also linked EphA2 with p53. In our present study, we examined EphA2 and p53 status (both expression and full-length mutation status) in 6 ovarian cell lines and 79 human ovarian cancers to determine potential associations. EphA2 was overexpressed in 80% of ovarian cancer cell lines and in 75% of clinical specimens. In particular, high levels of EphA2 occurred in 91% of tumors with p53 null mutations compared to 68% in tumors with wild-type or missense mutations (p = 0.027). EphA2 expression did not relate to critical versus noncritical site missense p53 mutations or the location of mutations on specific p53 exons. We also demonstrated that while EphA2 and p53 can provide independent information regarding clinical status, the combination of EphA2 and p53 status can predict poor clinical outcome. In particular, the combination of EphA2 overexpression and p53 null status was associated with decreased overall patient survival and related to increased incidence of ascites and distant metastasis. Taken together, these data indicate a complex relationship between EphA2 and p53 that appears to regulate EphA2 expression and clinical outcome.",
keywords = "Epha2, Null mutations, Ovarian carcinoma, P53, Tyrosine kinase",
author = "Merritt, {William M.} and Thaker, {Premal H.} and Landen, {Charles N.} and Deavers, {Michael T.} and Fletcher, {Mavis S.} and Lin, {Yvonne G.} and Han, {Liz Y.} and Kamat, {Aparna A.} and Rosemarie Schmandt and Gershenson, {David M.} and Kinch, {Michael S.} and Sood, {Anil K.}",
note = "Funding Information: Anderson Cancer Center SPORE in Ovarian The tumor suppressor gene, p53, critically controls apoptotic pathways.10-12 Previous Carcinoma #2P50CA083639, awarded to studies have linked p53 with EphA2 expression. For example, EphA2 expression is regulated A.K.S. This research was funded in part by the by p53 family members, which recognize a response element in the EphA2 promoter.13 NIH T32 grant (CA101642-01) to W.M.M. Likewise, preclinical studies have linked p53 and EphA2 expression with other cellular and the Department of Defense Grant stimuli.14-16 Many cancers, including ovarian cancer, frequently demonstrate altered #W81XW{\textcopyright}H-2040-0016-0 2L27A; DanEd Sth eB UOniSveCrsEityCEexpression or function of p53.17-23 In light of the independent links among EphA2 and SPORE in Ovarian Carcinomaof Texas MDAnderson Cancer Center p53 in cancer, we sought to determine potential links between these two targets in ovarian #2P50CA083639, awarded to A.K.S. cancer. In our present study, we demonstrate that p53 status does indeed relate to EphA2 overexpression in cancer. We expand upon knowledge that p53 and EphA2 can provide independent information about disease status by demonstrating that the combination of EphA2 overexpression and p53 status together can identify the most aggressive forms of the disease.",
year = "2006",
month = oct,
doi = "10.4161/cbt.5.10.3225",
language = "English (US)",
volume = "5",
pages = "1357--1360",
journal = "Cancer Biology and Therapy",
issn = "1538-4047",
publisher = "Landes Bioscience",
number = "10",
}