2010
DOI: 10.1155/2010/568938
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Targeting the Epidermal Growth Factor Receptor in Epithelial Ovarian Cancer: Current Knowledge and Future Challenges

Abstract: The epidermal growth factor receptor is overexpressed in up to 60% of ovarian epithelial malignancies. EGFR regulates complex cellular events due to the large number of ligands, dimerization partners, and diverse signaling pathways engaged. In ovarian cancer, EGFR activation is associated with increased malignant tumor phenotype and poorer patient outcome. However, unlike some other EGFR-positive solid tumors, treatment of ovarian tumors with anti-EGFR agents has induced minimal response. While the amount of i… Show more

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Cited by 120 publications
(118 citation statements)
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References 202 publications
(195 reference statements)
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“…EGFR is considered to be a key therapeutic target in many types of cancer. However, for reasons that are still unclear, treatment of EOC patients with anti-EGFR results in a very poor response and is not correlated to EGFR expression (Siwak et al, 2010). Therefore, there is an urgent need to further understand the relationships between the tumor microenvironment, EGFR activation and disease outcome in ovarian cancer.…”
Section: Introductionmentioning
confidence: 99%
“…EGFR is considered to be a key therapeutic target in many types of cancer. However, for reasons that are still unclear, treatment of EOC patients with anti-EGFR results in a very poor response and is not correlated to EGFR expression (Siwak et al, 2010). Therefore, there is an urgent need to further understand the relationships between the tumor microenvironment, EGFR activation and disease outcome in ovarian cancer.…”
Section: Introductionmentioning
confidence: 99%
“…Although we have demonstrated a modest correlation between EGFR and LAMP-1 expression in ovarian cancer tissue cores, it is important to note that increased expression of EGFR is not always predictive of therapeutic responses to receptor-targeted therapies. This has been demonstrated in both ovarian and colorectal cancers (12,52). Clinical trials performed using an EGFR monoclonal antibody for the treatment of receptor-positive cancers did not demonstrate clinical efficacy as a monoclonal antibody therapy, further illustrating the difficulty of predicting antibody responses based on overexpression alone (53).…”
Section: Discussionmentioning
confidence: 99%
“…Studies illustrate overamplification of the EGFR gene in between 4% and 22% of ovarian cancers, with aberrant protein expression in up to 60% of ovarian malignancies (10 -12). Aberrant EGFR expression has been associated with high tumor grade, increased cancerous cell proliferation, and poorer patient outcomes (12)(13)(14)(15). Gene amplification and the overexpression of other EGFR family members such as Her2 and ErbB3 have also been reported in epithelial ovarian cancers (15).…”
mentioning
confidence: 99%
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“…TKIs combined with cytotoxic chemotherapy, anti-angiogenic therapy, or hormonal therapy have also shown limited clinical efficacy and in some cases excessive toxicity (Campos et al 2010, Chambers et al 2010, Nimeiri et al 2008, Vasey et al 2008. The reason behind the relative failure of EGFR targeted therapies is not understood, but may be related to constitutive activation of downstream pathways, overexpression of ligands, or activation of alternative signaling pathways (reviewed in (Bianco et al 2007, Siwak et al 2010). Despite the promising preclinical results based on the amplification data, these therapeutic agents cannot be recommended outside of a clinical trial setting for the treatment of ovarian cancer.…”
Section: Epidermal Growth Factor Receptorsmentioning
confidence: 99%