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uploaded 2 May 2013
Abstract: Ovarian
carcinoma (OC) is the most lethal gynecological malignancy. Response to
platinum-based chemotherapy is poor in some patients and, thus, current
research is focusing on new therapy options. The various histological
types of OC are characterized by distinctive molecular genetic
alterations that are relevant for ovarian tumorigenesis. The
understanding of these molecular pathways is essential for the
development of novel therapeutic strategies.
Purpose: We want to
give an overview on the molecular genetic changes of the
histopathological types of OC and their role as putative therapeutic
targets.
In Depth Review of Existing Data: In 2012, the vascular
endothelial growth factor (VEGF) inhibitor, bevacizumab, was approved
for OC treatment. Bevacizumab has shown promising results as single
agent and in combination with conventional chemotherapy, but its target
is not distinctive when analyzed before treatment. At present, mammalian
target of rapamycin (mTOR) inhibitors, poly-ADP-ribose polymerase
(PARP) inhibitors and components of the EGFR pathway are in the focus of
clinical research. Interestingly, some phytochemical substances show
good synergistic effects when used in combination with chemotherapy.
Conclusion:
Ongoing studies of targeted agents in conjunction with chemotherapy
will show whether there are alternative options to bevacizumab available
for OC patients. Novel targets which can be assessed before therapy to
predict efficacy are needed. The assessment of therapeutic targets is
continuously improved by molecular pathological analyses on tumor
tissue. A careful selection of patients for personalized treatment will
help to reduce putative side effects and toxicity.
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