¹⁸F-FDG PET/CT 用于新辅助治疗三阴性乳腺癌早期疗效评估:化疗方案的影响。
¹⁸F-FDG PET/CT for the Early Evaluation of Response to Neoadjuvant Treatment in Triple-Negative Breast Cancer: Influence of the Chemotherapy Regimen.
机构信息
Department of Nuclear Medicine, APHP, Saint-Louis Hospital, Paris, France University Paris-Diderot, PRES Paris Cité, INSERM/CNRS UMR944/7212, Paris, France
Department of Biostatistics and Information, APHP, Saint-Louis Hospital, Paris, France.
出版信息
J Nucl Med. 2016 Apr;57(4):536-43. doi: 10.2967/jnumed.115.163907. Epub 2015 Dec 23.
UNLABELLED
Patients with triple-negative breast cancer (TNBC) have poor outcome when pathologic complete response (pCR) is not reached after neoadjuvant chemotherapy. Early prediction would be helpful. We evaluated the association between metabolic response after 2 cycles of neoadjuvant chemotherapy, pCR, and outcome in patients receiving 2 different anthracycline-based regimens (conventional and intensified).
METHODS
Of 77 consecutive TNBC patients, 23 received EC-D (4 cycles of epirubicin + cyclophosphamide followed by 4 cycles of docetaxel at conventional doses) and 55 received a dose-intensified, dose-dense concomitant regimen of epirubicin + cyclophosphamide (historically called SIM) for 6 cycles. PET/CT with (18)F-FDG was performed at baseline and after 2 cycles of neoadjuvant chemotherapy. The associations between clinical factors, biologic factors, early metabolic change, pCR, and event-free survival (EFS) were examined (log-rank test).
RESULTS
Of the 78 patients, 29 (37%) achieved pCR. The change in SUVmax (∆SUVmax) after 2 cycles was more pronounced in patients who achieved pCR (-72% vs. -42%;P< 0.0001). ∆SUVmax was more pronounced under SIM than under EC-D (-68% vs. -35%, P= 0.009), and there was a trend for a higher pCR rate (44% vs. 22%, P= 0.078). Twenty-two patients relapsed and 10 of them died (median follow-up, 34 mo). pCR was associated with EFS (log-rank, P= 0.001). ∆SUVmax was also significantly associated with EFS both in patients receiving SIM (P= 0.028) and in those receiving EC-D (P= 0.021). The optimal ∆SUVmax for predicting pCR and EFS was, however, specific to the treatment regimen. EFS was not associated with tumor grade (P= 0.98), histologic subtype (P= 0.17), or clinical stage (P= 0.097).
CONCLUSION
Early metabolic change during neoadjuvant chemotherapy can predict pathologic response and EFS in TNBC patients under different chemotherapy regimens. However, the metabolic response varies with the type of chemotherapy.
背景
新辅助化疗后未达到病理完全缓解(pCR)的三阴性乳腺癌(TNBC)患者预后较差。早期预测将有所帮助。我们评估了新辅助化疗 2 周期后代谢反应与 pCR 以及接受两种不同蒽环类药物方案(常规和强化)治疗的患者结局之间的关系。
方法
77 例连续 TNBC 患者中,23 例接受 EC-D(4 周期表柔比星+环磷酰胺,随后 4 周期多西他赛常规剂量),55 例接受强化、剂量密集的表柔比星+环磷酰胺同期方案(历史上称为 SIM)6 周期。新辅助化疗前和 2 周期后进行 PET/CT 检查,采用(18)F-FDG。检查临床因素、生物学因素、早期代谢变化、pCR 和无事件生存(EFS)之间的相关性(log-rank 检验)。
结果
78 例患者中,29 例(37%)达到 pCR。达到 pCR 的患者 SUVmax 变化(∆SUVmax)更明显(-72%对-42%;P<0.0001)。SIM 组比 EC-D 组更明显(-68%对-35%,P=0.009),且 pCR 率有升高趋势(44%对 22%,P=0.078)。22 例患者复发,10 例死亡(中位随访 34 个月)。pCR 与 EFS 相关(log-rank,P=0.001)。∆SUVmax 在接受 SIM 和 EC-D 的患者中与 EFS 显著相关(P=0.028 和 P=0.021)。但预测 pCR 和 EFS 的最佳∆SUVmax 是特定于治疗方案的。EFS 与肿瘤分级(P=0.98)、组织学亚型(P=0.17)或临床分期(P=0.097)无关。
结论
新辅助化疗期间的早期代谢变化可预测不同化疗方案下 TNBC 患者的病理反应和 EFS。然而,代谢反应随化疗类型而变化。
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