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Early Prediction and Evaluation of Breast Cancer Response to Neoadjuvant Chemotherapy Using Quantitative DCE-MRI

机译:定量DCE-MRI对乳腺癌新辅助化疗反应的早期预测和评估

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The purpose is to compare quantitative dynamic contrast-enhanced (DCE) magnetic resonance imaging (MRI) metrics with imaging tumor size for early prediction of breast cancer response to neoadjuvant chemotherapy (NACT) and evaluation of residual cancer burden (RCB). Twenty-eight patients with 29 primary breast tumors underwent DCE-MRI exams before, after one cycle of, at midpoint of, and after NACT. MRI tumor size in the longest diameter (LD) was measured according to the RECIST (Response Evaluation Criteria In Solid Tumors) guidelines. Pharmacokinetic analyses of DCE-MRI data were performed with the standard Tofts and Shutter-Speed models (TM and SSM). After one NACT cycle the percent changes of DCE-MRI parameters K trans (contrast agent plasma/interstitium transfer rate constant), v e (extravascular and extracellular volume fraction), k ep (intravasation rate constant) , and SSM-unique τ i (mean intracellular water lifetime) are good to excellent early predictors of pathologic complete response (pCR) vs. non-pCR, with univariate logistic regression C statistics value in the range of 0.804 to 0.967. v e values after one cycle and at NACT midpoint are also good predictors of response, with C ranging 0.845 to 0.897. However, RECIST LD changes are poor predictors with C = 0.609 and 0.673, respectively. Post-NACT K trans , τ i , and RECIST LD show statistically significant ( P .05) correlations with RCB. The performances of TM and SSM analyses for early prediction of response and RCB evaluation are comparable. In conclusion, quantitative DCE-MRI parameters are superior to imaging tumor size for early prediction of therapy response. Both TM and SSM analyses are effective for therapy response evaluation. However, the τ i parameter derived only with SSM analysis allows the unique opportunity to potentially quantify therapy-induced changes in tumor energetic metabolism.
机译:目的是将定量动态对比增强(DCE)磁共振成像(MRI)指标与成像肿瘤大小进行比较,以早期预测乳腺癌对新辅助化疗(NACT)的反应并评估残余癌症负荷(RCB)。 28例29例原发性乳腺肿瘤患者在NACT之前,一个周期之后,中点和之后接受了DCE-MRI检查。根据RECIST(实体瘤反应评估标准)指南测量最长直径(LD)的MRI肿瘤大小。 DCE-MRI数据的药代动力学分析是使用标准Tofts和Shutter-Speed模型(TM和SSM)进行的。在一个NACT周期后,DCE-MRI参数K trans(造影剂血浆/间质转移速率常数),ve(血管外和细胞外体积分数),kep(血管浸润率常数)和SSM唯一τi(平均值)的百分比变化细胞内水的寿命)是病理完全反应(pCR)与非pCR的极好早期预测指标,单因素logistic回归C统计值在0.804至0.967之间。一个周期后和NACT中点的v e值也可以很好地预测反应,C的范围为0.845至0.897。但是,RECIST LD的变化分别是C = 0.609和0.673的不良预测指标。 NACT后的K trans,τi和RECIST LD与RCB具有统计显着性(P <.05)相关性。 TM和SSM分析在响应的早期预测和RCB评估方面的性能可比。总之,对于早期预测治疗反应,定量DCE-MRI参数优于成像肿瘤大小。 TM分析和SSM分析对治疗反应评估均有效。但是,仅通过SSM分析得出的τi参数提供了独特的机会来潜在地量化治疗诱导的肿瘤能量代谢变化。

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