首页> 外文期刊>International Journal of Radiation Oncology, Biology, Physics >Can the analysis of ERCC1 expression contribute to individualized therapy in nasopharyngeal carcinoma?
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Can the analysis of ERCC1 expression contribute to individualized therapy in nasopharyngeal carcinoma?

机译:ERCC1表达的分析能否有助于鼻咽癌的个体化治疗?

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PURPOSE: To analyze the expression of excision repair cross-complementation group 1 (ERCC1) protein in predicting the clinical outcome of nasopharyngeal carcinoma (NPC). METHODS AND MATERIALS: The histologic specimens of 258 patients with Stage III to IVB nonkeratinizing NPC who were treated with radiotherapy alone (Group I) or concurrent-adjuvant chemoradiotherapy (Group II) were retrieved. Immunostaining on ERCC1 protein was performed. The relationship of ERCC1 expression and clinical outcomes was analyzed. RESULTS: The median ERCC1 score (proportion score of positively stained cells times intensity) was 200 (range, 0-300), and ERCC1 expression was defined as high if the score was above the median. In Group I high-score tumor had a statistically lower locoregional failure-free rate (LRFFR) compared with low-score tumor (p < 0.05) but not distant failure-free rate (DFFR) and overall survival (OS). In Group II no statistically differences were noted in LRFFR, DFFR and OS with regard to the ERCC1 expression. Resistance to cisplatin-containing chemotherapy in high-ERCC1 score tumor was not observed in Group II. Interestingly, low-score tumor in Group I achieved similar local and distant control compared with Group II. Multivariate analysis showed that ERCC1 score was an independent prognostic factor in LRFFR (p < 0.05) and approached statistical significance in failure-free survival (p = 0.08) and OS (p = 0.07). Tumor with high ERCC1 score had a 2-fold (95% confidence interval, 1.02-3.85) increased risk of locoregional failure. This may imply an association of ERCC1 expression with the repair of radiation damage. CONCLUSIONS: High ERCC1 expression predicts poor locoregional control in NPC. Chemotherapy response is not affected by ERCC1 expression. Further validation is required.
机译:目的:分析切除修复交叉互补1族(ERCC1)蛋白在预测鼻咽癌(NPC)临床结局中的表达。方法和材料:取258例单独放疗(I组)或同期辅助放化疗(II组)的III至IVB期非角化NPC患者的组织学标本。对ERCC1蛋白进行了免疫染色。分析了ERCC1表达与临床结果的关系。结果:ERCC1得分的中位数(阳性染色细胞的比例得分乘以强度)为200(范围为0-300),如果得分高于中位数,则ERCC1表达被定义为高。在第一组中,高评分肿瘤的局部无衰竭率(LRFFR)低于低评分肿瘤(p <0.05),但远距无衰竭率(DFFR)和总生存率(OS)则没有统计学意义。在第二组中,关于ERCC1表达,LRFFR,DFFR和OS没有统计学差异。在第二组中未观察到高ERCC1评分肿瘤对含顺铂化疗的耐药性。有趣的是,与第二组相比,第一组的低分肿瘤获得了相似的局部和远距离控制。多变量分析表明,ERCC1评分是LRFFR的独立预后因素(p <0.05),并且在无失败生存率(p = 0.08)和OS(p = 0.07)方面具有统计学意义。 ERCC1评分高的肿瘤局部区域衰竭的风险增加了2倍(95%置信区间,1.02-3.85)。这可能暗示ERCC1表达与辐射损伤的修复有关。结论:ERCC1高表达预示着鼻咽癌的局部区域控制不良。化疗反应不受ERCC1表达的影响。需要进一步验证。

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