首页> 外文期刊>Journal of the National Cancer Institute >Long-term outcomes of invasive ipsilateral breast tumor recurrences after lumpectomy in NSABP B-17 and B-24 randomized clinical trials for DCIS.
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Long-term outcomes of invasive ipsilateral breast tumor recurrences after lumpectomy in NSABP B-17 and B-24 randomized clinical trials for DCIS.

机译:NSABP B-17和B-24的DCIS随机临床试验中,肿块切除术后浸润性同侧乳腺肿瘤复发的长期结果。

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BACKGROUND: Ipsilateral breast tumor recurrence (IBTR) is the most common failure event after lumpectomy for ductal carcinoma in situ (DCIS). We evaluated invasive IBTR (I-IBTR) and its influence on survival among participants in two National Surgical Adjuvant Breast and Bowel Project (NSABP) randomized trials for DCIS. METHODS: In the NSABP B-17 trial (accrual period: October 1, 1985, to December 31, 1990), patients with localized DCIS were randomly assigned to the lumpectomy only (LO, n = 403) group or to the lumpectomy followed by radiotherapy (LRT, n = 410) group. In the NSABP B-24 double-blinded, placebo-controlled trial (accrual period: May 9, 1991, to April 13, 1994), all accrued patients were randomly assigned to LRT+ placebo, (n=900) or LRT + tamoxifen (LRT + TAM, n = 899). Endpoints included I-IBTR, DCIS-IBTR, contralateral breast cancers (CBC), overall and breast cancer-specific survival, and survival after I-IBTR. Median follow-up was 207 months for the B-17 trial (N = 813 patients) and 163 months for the B-24 trial (N = 1799 patients). RESULTS: Of 490 IBTR events, 263 (53.7%) were invasive. Radiation reduced I-IBTR by 52% in the LRT group compared with LO (B-17, hazard ratio [HR] of risk of I-IBTR = 0.48, 95% confidence interval [CI] = 0.33 to 0.69, P < .001). LRT + TAM reduced I-IBTR by 32% compared with LRT + placebo (B-24, HR of risk of I-IBTR = 0.68, 95% CI = 0.49 to 0.95, P = .025). The 15-year cumulative incidence of I-IBTR was 19.4% for LO, 8.9% for LRT (B-17), 10.0% for LRT + placebo (B-24), and 8.5% for LRT + TAM. The 15-year cumulative incidence of all contralateral breast cancers was 10.3% for LO, 10.2% for LRT (B-17), 10.8% for LRT + placebo (B-24), and 7.3% for LRT + TAM. I-IBTR was associated with increased mortality risk (HR of death = 1.75, 95% CI = 1.45 to 2.96, P < .001), whereas recurrence of DCIS was not. Twenty-two of 39 deaths after I-IBTR were attributed to breast cancer. Among all patients (with or without I-IBTR), the 15-year cumulative incidence of breast cancer death was 3.1% for LO, 4.7% for LRT (B-17), 2.7% for LRT + placebo (B-24), and 2.3% for LRT + TAM. CONCLUSIONS: Although I-IBTR increased the risk for breast cancer-related death, radiation therapy and tamoxifen reduced I-IBTR, and long-term prognosis remained excellent after breast-conserving surgery for DCIS.
机译:背景:同侧乳腺肿瘤复发(IBTR)是输卵管癌原位切除术(DCIS)后最常见的失败事件。我们在两项针对DCIS的国家外科辅助性乳房和肠项目(NSABP)随机试验中,评估了侵入性IBTR(I-IBTR)及其对参与者生存率的影响。方法:在NSABP B-17试验(应计期:1985年10月1日至1990年12月31日)中,将具有局限性DCIS的患者随机分配为仅行肿块切除术(LO,n = 403)组或随后进行的肿块切除术。放疗(LRT,n = 410)组。在NSABP B-24双盲,安慰剂对照试验中(应计期:1991年5月9日至1994年4月13日),所有应计患者均随机分配为LRT +安慰剂(n = 900)或LRT +他莫昔芬( LRT + TAM,n = 899)。终点包括I-IBTR,DCIS-IBTR,对侧乳腺癌(CBC),总体和乳腺癌特异性生存率以及I-IBTR后生存率。 B-17试验的中位随访时间为207个月(N = 813例患者),B-24试验的中位随访时间为163个月(N = 1799例)。结果:在490例IBTR事件中,有263例(53.7%)是浸润性的。与LO相比,LRT组的辐射使I-IBTR降低了52%(B-17,I-IBTR风险的危险比[HR] = 0.48,95%置信区间[CI] = 0.33至0.69,P <.001 )。与LRT +安慰剂相比,LRT + TAM使I-IBTR降低了32%(B-24,I-IBTR风险的HR = 0.68,95%CI = 0.49至0.95,P = .025)。 I-IBTR的15年累积发生率:LO为19.4%,LRT(B-17)为8.9%,LRT +安慰剂(B-24)为10.0%,LRT + TAM为8.5%。所有对侧乳腺癌的15年累积发生率分别为LO的10.3%,LRT(B-17)的10.2%,LRT +安慰剂(B-24)的10.8%,LRT + TAM的7.3%。 I-IBTR与死亡风险增加相关(死亡HR = 1.75,95%CI = 1.45至2.96,P <.001),而DCIS的复发则没有。 I-IBTR后39例死亡中有22例归因于乳腺癌。在所有患者(有或无I-IBTR)中,LO的15年乳腺癌死亡累积发生率分别为:LO 3.1%,LRT(B-17)4.7%,LRT +安慰剂(B-24)2.7%, LRT + TAM占2.3%。结论:尽管I-IBTR增加了乳腺癌相关死亡的风险,但是放射治疗和他莫昔芬降低了I-IBTR,并且DCIS保乳手术后的长期预后仍然很好。

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