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首页> 外文期刊>The Journal of Nuclear Medicine >Preclinical PERCIST and 25% of SUVmax Threshold: Precision Imaging of Response to Therapy in Co-clinical F-18-FDG PET Imaging of Triple-Negative Breast Cancer Patient-Derived Tumor Xenografts
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Preclinical PERCIST and 25% of SUVmax Threshold: Precision Imaging of Response to Therapy in Co-clinical F-18-FDG PET Imaging of Triple-Negative Breast Cancer Patient-Derived Tumor Xenografts

机译:临床前栖息术和25%的Suvmax阈值:对三重阴性乳腺癌患者衍生的肿瘤异种移植物的共临床F-18-FDG宠物成像进行响应的精确成像

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Numerous recent works highlight the limited utility of established tumor cell lines in recapitulating the heterogeneity of tumors in patients. More realistic preclinical cancer models are thought to be provided by transplantable, patient-derived xenografts (PDXs). The inter- and intratumor heterogeneity of PDXs, however, presents several challenges in developing optimal quantitative pipelines to assess response to therapy. The objective of this work was to develop and optimize image metrics for F-18-FDG PET to assess response to combination docetaxel and carboplatin therapy in a co-clinical trial involving triple-negative breast cancer PDXs. We characterized the reproducibility of standardized uptake value (SUV) metrics to assess response to therapy, and we optimized a preclinical PERCIST paradigm to complement clinical standards. Considerations in this effort included variability in tumor growth rate and tumor size, solid tumors versus tumor heterogeneity and a necrotic phenotype, and optimal selection of tumor slices versus whole tumor. Methods: A test-retest protocol was implemented to optimize the reproducibility of F-18-FDG PET SUV thresholds, SUVpeak metrics, and preclinical PERCIST parameters. In assessing response to therapy, F-18-FDG PET imaging was performed at baseline and 4 d after therapy. The reproducibility, accuracy, variability, and performance of imaging metrics to assess response to therapy were determined. We defined an index called the Quantitative Response Assessment Score to integrate parameters of prediction and precision and thus aid in selecting the optimal image metric to assess response to therapy. Results: Our data suggest that a threshold of 25% of SUVmax (SUV25) was highly reproducible (<9% variability). The concordance and reproducibility of preclinical PERCIST were maximized at alpha = 0.7 and beta = 2.8 and exhibited a high correlation with SUV25 measures of tumor uptake, which in turn correlated with the SUV of metabolic tumor. Conclusion: The Quantitative Response Assessment Score favors SUV25 followed by SUVpeak for a sphere with a volume of 14 mm(3) (SUVP14) as optimal metrics of response to therapy. Additional studies are warranted to fully characterize the utility of SUV25 and preclinical PERCIST SUVP14 as image metrics for response to therapy across a wide range of therapeutic regimens and PDX models.
机译:近期作品突出了已建立的肿瘤细胞系在重新携带患者肿瘤的异质性时的有限效用。认为更现实的临床前癌症模型是通过可移植的患者衍生的异种移植物(PDX)提供的。然而,PDX的间和肿瘤内异质性具有若干挑战在开发最佳的定量管道中以评估治疗的反应。这项工作的目的是为F-18-FDG宠物开发和优化图像指标,以评估对Codetaxel和Carboplatin治疗组合的反应,涉及三阴性乳腺癌PDX的共同临床试验。我们表征了标准化摄取值(SUV)指标的重现性,以评估对治疗的反应,我们优化了一种临床前的Percist范式来补充临床标准。在这项工作中的考虑因素包括肿瘤生长速率和肿瘤大小的可变性,实体瘤与肿瘤异质性和坏死表型,以及最佳选择肿瘤切片与整个肿瘤。方法:实施了测试重新测试的协议,以优化F-18-FDG PET SUV阈值,SUVPEAK度量和临床前Percist参数的再现性。在评估对治疗的反应时,在治疗后在基线和4 d处进行F-18-FDG宠物成像。确定了成像度量来评估治疗响应的成像度量的再现性,准确性,可变性和性能。我们定义了称为定量响应评估评分的索引,以集成预测和精度的参数,从而有助于选择最佳图像度量来评估对治疗的反应。结果:我们的数据表明,25%的Suvmax(SUV25)的阈值高度可重复(<9%的变化)。临床前切除症的一致性和再现性在α= 0.7和β= 2.8时最大化,并与肿瘤摄取的SUV25测量表现出高的相关性,其又与代谢肿瘤的SUV相关。结论:定量响应评估评分得到了SUV25,其次是体积为14mm(3)(SUVP14)的球体的SUVPEAK作为对治疗的最佳度量。需要进行额外的研究以充分表征SUV25和临床前Percist SUVP14的效用作为图像指标,以应对跨各种治疗方案和PDX模型的治疗。

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