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首页> 外文期刊>Annals of oncology: official journal of the European Society for Medical Oncology >Breast cancer recurrence dynamics following adjuvant CMF is consistent with tumor dormancy and mastectomy-driven acceleration of the metastatic process.
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Breast cancer recurrence dynamics following adjuvant CMF is consistent with tumor dormancy and mastectomy-driven acceleration of the metastatic process.

机译:辅助CMF后乳腺癌的复发动态与肿瘤休眠和乳房切除术驱动的转移过程加速一致。

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摘要

PURPOSE: The aim of this study was to better understand human breast cancer biology by studying how the timing of metastasis following primary resection is affected by adjuvant CMF (cyclophoshamide, methotrexate, 5-fluorouracil) chemotherapy. PATIENTS AND METHODS: Discrete hazards of recurrence and recurrence risk reductions for treated patients relative to controls were analyzed for all patients enrolled in two separate randomized clinical trials [study 1 (386 women): no further treatment versus 12 cycles of CMF; study 2 (459 women): six versus 12 cycles of CMF] and a historical group (396 women: surgery alone) of axillary node-positive patients undergoing mastectomy. RESULTS: (i) Nearly all CMF benefit occurs during the first 4 years following resection/chemotherapy. (ii) The CMF recurrence rate reduction is largely restricted to two specific spans. These temporally separate recurrence clusters occur during the first and third year of follow-up, while the second-year recurrences are weakly affected. (iii) Prolonging adjuvant treatment from 6 to 12 months partially alters this recurrence timing, without appreciably affecting the overall recurrence rate. (iv) These effects upon the dynamics of post-resection occurrence are menopausal status-independent. CONCLUSIONS: At least two different therapeutically vulnerable proliferative events, resulting in clinical appearance of two metastasis temporally distinct clusters of post-resection cancer recurrence, apparently occur during the administration of adjuvant chemotherapy. Metastases that transpire outside of these temporal windows are refractory to adjuvant therapy. The dynamics of both post-treatment recurrence risk and CMF effectiveness are similar for both pre- and postmenopausal women, suggesting that post-resection mechanisms by which chemotherapy prevents metastases are similar, but of different magnitude in pre- and postmenopausal women. These findings are consistent with a metastasis model that includes tumor dormancy in specific micrometastatic phases (single cells and avascular foci) and with the acceleration of the metastatic process by the surgical resection of the primary breast cancer.
机译:目的:本研究的目的是通过研究辅助切除术(CMF)(环磷酰胺,甲氨蝶呤,5-氟尿嘧啶)如何影响一次切除后转移的时机,从而更好地了解人类乳腺癌生物学。患者和方法:对参加两项单独的随机临床试验的所有患者进行分析,分析了相对于对照组而言治疗后患者的离散复发风险和复发风险降低[研究1(386名女性):无进一步治疗与12个周期的CMF;研究2(459名妇女):CMF周期为12周期与12周期相比)和历史组(396名妇女:仅接受手术)行乳房切除术的腋窝淋巴结阳性患者。结果:(i)几乎所有CMF获益都发生在切除/化学疗法后的前4年。 (ii)CMF复发率的降低主要限于两个特定范围。这些在时间上分开的复发群发生在随访的第一年和第三年,而第二年的复发受到的影响较小。 (iii)将辅助治疗延长6到12个月可以部分改变这种复发时机,而不会显着影响总体复发率。 (iv)这些对切除术后发生动力学的影响与绝经状态无关。结论:至少有两个不同的治疗上脆弱的增生事件,导致在切除辅助癌的复发过程中出现了两个在时间上截然不同的簇转移的临床表现,这显然是在辅助化疗期间发生的。在这些颞窗外散发的转移对于辅助治疗是难治的。绝经前和绝经后妇女的治疗后复发风险和CMF有效性的变化相似,这表明切除后通过化学疗法预防转移的机制相似,但绝经前和绝经后妇女的幅度不同。这些发现与包括特定微转移阶段(单细胞和无血管灶)中的肿瘤休眠在内的转移模型以及通过原发性乳腺癌的手术切除加速转移过程相一致。

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