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MRE11 expression is predictive of cause-specific survival following radical radiotherapy for muscle-invasive bladder cancer.

机译:MRE11表达可预示根治性放射疗法治疗肌肉浸润性膀胱癌后特定原因的生存。

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摘要

Radical radiotherapy and surgery achieve similar cure rates in muscle-invasive bladder cancer, but the choice of which treatment would be most beneficial cannot currently be predicted for individual patients. The primary aim of this study was to assess whether expression of any of a panel of DNA damage signaling proteins in tumor samples taken before irradiation could be used as a predictive marker of radiotherapy response, or rather was prognostic. Protein expression of MRE11, RAD50, NBS1, ATM, and H2AX was studied by immunohistochemistry in pretreatment tumor specimens from two cohorts of bladder cancer patients (validation cohort prospectively acquired) treated with radical radiotherapy and one cohort of cystectomy patients. In the radiotherapy test cohort (n = 86), low tumor MRE11 expression was associated with worse cancer-specific survival compared with high expression [43.1% versus 68.7% 3-year cause-specific survival (CSS), P = 0.012] by Kaplan-Meier analysis. This was confirmed in the radiotherapy validation cohort (n = 93; 43.0% versus 71.2%, P = 0.020). However, in the cystectomy cohort (n = 88), MRE11 expression was not associated with cancer-specific survival, commensurate with MRE11 being a predictive marker. High MRE11 expression in the combined radiotherapy cohort had a significantly better cancer-specific survival compared with the high-expression cystectomy cohort (69.9% versus 53.8% 3-year CSS, P = 0.021). In this validated immunohistochemistry study, MRE11 protein expression was shown and confirmed as a predictive factor associated with survival following bladder cancer radiotherapy, justifying its inclusion in subsequent trial designs. MRE11 expression may ultimately allow patient selection for radiotherapy or cystectomy, thus improving overall cure rates.
机译:根治性放射疗法和外科手术在肌肉浸润性膀胱癌中可达到相似的治愈率,但目前尚无法预测个别患者选择哪种治疗最有益。这项研究的主要目的是评估在放射线照射之前采集的肿瘤样品中一组DNA损伤信号传导蛋白的表达是否可以用作放射治疗反应的预测标记,或者是否具有预后性。通过免疫组织化学研究了来自两个接受放疗的膀胱癌患者(预期获得的验证队列)和一个接受膀胱切除术患者的队列治疗前肿瘤标本中MRE11,RAD50,NBS1,ATM和H2AX的蛋白表达。在放射治疗试验队列中(n = 86),Kaplan的低肿瘤MRE11表达与较差的癌症特异性存活率相关,而与高表达相比[43.1%对68.7%的3年原因特异性存活率(CSS),P = 0.012] -Meier分析。这在放疗验证队列中得到了证实(n = 93; 43.0%对71.2%,P = 0.020)。但是,在膀胱切除术队列(n = 88)中,MRE11表达与癌症特异性生存率无关,与MRE11是预测指标相对应。与高表达膀胱切除术队列相比,联合放疗队列中高MRE11表达具有更好的癌症特异性生存率(69.9%比3年CSS的53.8%,P = 0.021)。在这项经过验证的免疫组织化学研究中,MRE11蛋白的表达被证实并被确认为与膀胱癌放疗后生存相关的预测因素,证明其被纳入随后的试验设计中。 MRE11的表达可能最终允许患者选择放射治疗或膀胱切除术,从而提高总体治愈率。

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