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Reirradiation to the pelvis for recurrent rectal cancer

机译:再次照射骨盆治疗直肠癌

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摘要

Objectives This study investigated late toxicity and infield progression-free survival in patients with locally recurrent rectal cancer (LRRC) who had previously received irradiation to the pelvis. Methods Twenty-two patients were treated by reirradiation to the pelvis between January 2000 and August 2007. All patients received curative surgery with preoperative or postoperative chemoradiotherapy as an initial treatment. Five patients (23%) underwent surgical resection after reirradiation. The median follow-up duration was 20 months (range, 7-91 months). Results Two patients (9%) had grade-3 acute toxicity and eight patients (36%) had grade-3 to -4 late toxicity. The incidence of grade-3 to -4 late toxicity in the gastrointestinal and urinary system was 18% and 27%, respectively. Recurrent tumor location (axial or anterior) and surgical resection after reirradiation significantly influenced severe late toxicity (P=0.024 and P=0.039, respectively). In the 17 patients not undergoing surgery after reirradiation, median infield progression-free survival was 16 months. Reirradiation doses exceeding 50Gy αβ10 (equivalent dose in 2Gy fractions) significantly increased the infield progression-free survival (P=0.005). Conclusions Tumor location (axial or anterior) and surgery after reirradiation may increase severe late toxicity. In addition, an EQD2 exceeding 50Gy αβ10 may improve infield control.
机译:目的本研究调查了先前接受过骨盆照射的局部复发性直肠癌(LRRC)患者的后期毒性和无内野进展的生存率。方法2000年1月至2007年8月,对22例患者行骨盆再放射治疗。所有患者均接受根治性手术,其中术前或术后放化疗均作为初始治疗。五名患者(23%)在重新辐照后接受了手术切除。中位随访时间为20个月(范围7-91个月)。结果2例患者(9%)具有3级急性毒性,8例患者(36%)具有3至-4级晚期毒性。在胃肠道和泌尿系统中,3-4级晚期毒性的发生率分别为18%和27%。复发的肿瘤位置(轴向或前部)和再照射后的手术切除显着影响了严重的晚期毒性(分别为P = 0.024和P = 0.039)。在17位未接受再放射治疗的患者中,中位无进展进展生存期为16个月。超过50Gyαβ10的再照射剂量(相当于2Gy分数的剂量)显着提高了无内场生存率(P = 0.005)。结论肿瘤的位置(轴向或前向)和再次照射后的手术可能会增加严重的晚期毒性。另外,EQD2超过50Gyαβ10可以改善野外控制。

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