Thus, it is necessary to investigate different tumour types and stages in order to determine the role of amphiregulin for Cisplatin resistance. Further studies will determine
the impact of amphiregulin expression for therapy response and outcome in women with breast cancer. Figure 2 Schematic model of Amphiregulin signalling. Amphiregulin induced signaling of the EGFR/ERBB2 receptor tyrosine kinases in Cisplatin resistant MCF-7 cells. Ovarian cancer Clinicians have designated ovarian cancer a “”silent killer”" because, when diagnosed, the disease usually has already spread into the peritoneum [65]. If the cancer is diagnosed while confined to the ovary (localized stage), the 5-year survival rate is PLX3397 over 90%. In contrast, if ovarian cancer is diagnosed after it has metastasized (distant stage), the 5-year survival rate is below 30%. Unfortunately, most cases (68%) are diagnosed at the distant stage. Thus, ovarian cancer has a substantially shorter and more dramatic etiopathology than breast cancer: ovarian cancer is the most lethal gynecological cancer in the industrialized nations although its first occurrence has a satisfactory clinical response to platinum-based chemotherapy [10]. The reason is that more than 80% of the patients experience an early relapse [66]. The tumour usually reappears in OICR-9429 advanced stage or as metastatic
form of the disease (FIGO III/IV), which is treated in first line with cytoreductive surgery followed by chemotherapy doublets consisting of a Platinum-based compound combined with a Taxane. Target Selective Inhibitor Library Resistance to Platinum-containing compounds is a major Fossariinae obstacle in ovarian cancer therapy and the underlying mechanisms are not completely understood. Formation of a Cisplatin resistant phenotype after initial drug response usually is entailed with a lethal
course of the disease after a relapse [67]. Cellular defense to Cisplatin evolves as concerted action of growth factors, RTKs, MAPKs and other signal transduction pathways. The emergence of ovarian cancer proceeds with clinically diffuse symptoms [68]. Unfortunately, ovarian cancer is not contemporarily diagnosed because early symptoms like abdominal pain are not regarded as signs of a deadly disease by the patient. When symptoms aggravate, the patient often is already moribund. Ovarian cancer incidence peaks in the sixth and seventh life decade [67]. Approximately 5% of ovarian cancer cases have a hereditary background: women bear an increased risk of ovarian cancer if a first-degree relative suffers from (or died of) ovarian or breast cancer [69]. Therapeutic intervention of ovarian carcinomas can have different intentions, first, a curative approach intending the complete removal of the tumour and significant extension of survival time. To achieve this objective, severe side effects are accepted.