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FBXL7 Upregulation Predicts a Poor Prognosis and Associates with a Possible Mechanism for Paclitaxel Resistance in Ovarian Cancer

机译:FBXL7 Upregulation预测卵巢癌中可能具有紫杉醇抗性的可能机制差的预后和缔合机构差

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摘要

Paclitaxel (PTX) is a common regimen used to treat patients with ovarian cancer. Although approximately 60% of ovarian cancer patients exhibit a pathologic complete response (pCR), approximately 40% of patients appear to be insensitive to PTX adjuvant therapy. Thus, identifying a useful biomarker to predict pCR would be of great help to ovarian cancer patients who decide to receive PTX treatment. We found that FBXL7 was downregulated in OVSAHO (PTX-sensitive) but upregulated in KURAMOCHI (PTX-resistant) cells after PTX treatment at cytotoxic concentrations. Moreover, our data showed that the fold change of FBXL7 expression post-treatment with PTX was causally correlated with the 50% inhibitory concentrations (IC50) of PTX in a panel of ovarian cancer cell lines. In assessments of progression-free survival probability, high levels of FBXL7 transcript strongly predicted a poor prognosis and unfavorable response to PTX-based chemotherapy in patients with ovarian cancer. The knockdown of FBXL7 predominantly enhanced the cytotoxic effectiveness of PTX on the PTX-resistant KURAMOCHI cells. FBXL7 may be a useful biomarker for predicting complete pathologic response in ovarian cancer patients who decide to receive post-operative PTX therapy.
机译:紫杉醇(PTX)是一种用于治疗卵巢癌患者的共同方案。虽然卵巢癌患者的约60%表现出病理完全反应(PCR),患者的大约40%似乎是不敏感的PTX的辅助治疗。因此,识别有用的生物标记物来预测的pCR将是对谁决定接收PTX治疗卵巢癌患者有很大的帮助。我们发现,FBXL7在OVSAHO(PTX敏感)下调,但在KURAMOCHI(PTX耐)在细胞毒性浓度PTX治疗后细胞上调。此外,我们的数据表明,FBXL7表达后处理的用PTX的倍数变化是因果与卵巢癌细胞系的面板PTX的50%抑制浓度(IC 50)相关。在无进展生存概率的评估,高水平FBXL7成绩单的强烈预测卵巢癌患者的基于PTX-化疗预后差和不利的反应。 FBXL7的敲低主要增强PTX对耐PTX-KURAMOCHI细胞的细胞毒效果。 FBXL7可能是预测谁决定接受手术后PTX治疗卵巢癌患者病理完全缓解一个有用的生物标志物。

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