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MRI 分期的高危直肠癌新辅助化疗是否可替代或补充术前放化疗?

Neoadjuvant chemotherapy in MRI-staged high-risk rectal cancer in addition to or as an alternative to preoperative chemoradiation?

机构信息

Mount Vernon Cancer Centre, Mount Vernon Hospital, Northwood, UK.

Mount Vernon Cancer Centre, Mount Vernon Hospital, Northwood, UK.

出版信息

Ann Oncol. 2012 Oct;23(10):2517-2526. doi: 10.1093/annonc/mds010. Epub 2012 Feb 23.

Abstract

BACKGROUND

For patients with resectable rectal cancer chemoradiation (CRT) or short-course preoperative radiotherapy (SCPRT) reduces locoregional failure, without extending disease-free survival (DFS) or overall survival (OS). Compliance to postoperative adjuvant chemotherapy is poor. Neoadjuvant chemotherapy (NACT) offers an alternative strategy.

METHODS

A systematic computerised database search identified studies exploring NACT alone or NACT preceding/succeeding radiation. The primary outcome measure was pathological complete response (pCR). Secondary outcome measures included acute toxicity, surgical morbidity, circumferential resection margin, locoregional failure, DFS and OS.

RESULTS

Four case reports, 12 phase I/II studies, 4 randomised phase II and one randomised phase III study evaluated chemotherapy before CRT. Four prospective studies reviewed chemotherapy after CRT. Three phase II studies investigated chemotherapy using FOLFOX plus bevacizumab without radiotherapy. In 24 studies of 1271 patients, pCR varied from 7% to 36%, but with no impact on metastatic disease.

CONCLUSIONS

NACT before CRT delivers does not compromise CRT but has not increased pCR rates, R0 resection rate, improved DFS or reduced metastases. NACT following CRT is an interesting strategy, and the utility of NACT alone could be explored compared with SCPRT or CRT in selected patients with rectal cancer where the impact of radiotherapy on DFS and OS is marginal.

摘要

背景

对于可切除的直肠癌患者,放化疗(CRT)或短程术前放疗(SCPRT)可降低局部区域复发率,而不会延长无病生存期(DFS)或总生存期(OS)。术后辅助化疗的依从性较差。新辅助化疗(NACT)提供了一种替代策略。

方法

系统计算机数据库搜索确定了单独探索 NACT 或 NACT 之前/之后放射治疗的研究。主要观察指标为病理完全缓解(pCR)。次要观察指标包括急性毒性、手术发病率、环周切缘、局部区域失败、DFS 和 OS。

结果

四项病例报告、十二项 I/II 期研究、四项随机 II 期研究和一项随机 III 期研究评估了 CRT 前的化疗。四项前瞻性研究回顾了 CRT 后的化疗。三项 II 期研究调查了不联合放疗使用 FOLFOX 加贝伐单抗的化疗。在 1271 名患者的 24 项研究中,pCR 从 7%到 36%不等,但对转移性疾病没有影响。

结论

CRT 前的 NACT 不会影响 CRT,但并未增加 pCR 率、R0 切除率、改善 DFS 或减少转移。CRT 后的 NACT 是一种有趣的策略,并且可以在局部区域复发率较高的直肠癌患者中探索单独使用 NACT 与 SCPRT 或 CRT 的比较,因为放疗对 DFS 和 OS 的影响有限。

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