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首页> 外文期刊>Journal of Thoracic Disease >PET/CT evaluation of response to chemotherapy in non-small cell lung cancer: PET response criteria in solid tumors (PERCIST) versus response evaluation criteria in solid tumors (RECIST)
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PET/CT evaluation of response to chemotherapy in non-small cell lung cancer: PET response criteria in solid tumors (PERCIST) versus response evaluation criteria in solid tumors (RECIST)

机译:非小细胞肺癌对化疗反应的PET / CT评估:实体瘤的PET反应标准(PERCIST)与实体瘤的反应评估标准(RECIST)

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Background: 18 F-FDG PET/CT is increasingly used in evaluation of treatment response for patients with non-small cell lung cancer (NSCLC). There is a need for an accurate criterion to evaluate the effect and predict the prognosis. The aim of this study is to evaluate therapeutic response in NSCLC with comparing PET response criteria in solid tumors (PERCIST) to response evaluation criteria in solid tumors (RECIST) criteria on PET/CT. Methods: Forty-four NSCLC patients who received chemotherapy but no surgery were studied. Chemotherapeutic responses were evaluated using 18 F-FDG PET and CT according to the RECIST and PERCIST methodologies. PET/CT scans were obtained before chemotherapy and after 2 or 4-6 cycles’ chemotherapy. The percentage changes of tumor longest diameters and standardized uptake value (SUV) (corrected for lean body mass, SUL) before and after treatment were compared using paired t -test. The response was categorized into 4 levels according to RECIST and PERCIST: CR (CMR) =1, PR (PMR) =2, SD (SMD) =3, PD (PMD) =4. Pearson chi-square test was used to compare the proportion of four levels in RECIST and PERCIST. Finally the relationship between progression-free survival (PFS) and clinicopathologic parameters (such as TNM staging, percentage changes in diameters and SUL, RECIST and PERCIST results etc.) were evaluated using univariate and multivariate Cox proportional hazards regression method. Results: The difference of percentage changes between diameters and SUL was not significant using paired t -test ( t =–1.69, P=0.098). However the difference was statistically significant in the 40 cases without increasing SUL ( t =–3.31, P=0.002). The difference of evaluation results between RECIST and PERCIST was not significant by chi-square test (χ 2 =5.008, P=0.171). If RECIST evaluation excluded the new lesions which could not be found or identified on CT images the difference between RECIST and PERCIST was significant (χ 2 =11.759, P=0.007). Reduction rate of SUL peak (%), RECIST and PERCIST results were significant factors in univariate Cox analysis. But Multivariate Cox proportional hazards regression analysis demonstrated that only PERCIST was a significant factor for predicting DFS [hazard ratio (HR), 3.20; 95% (CI), 1.85-5.54; P0.001]. Conclusions: PERCIST and RECIST criteria have good consistency and PERCIST (or PET) is more sensitive in detecting complete remission (CR) and progression. PERCIST might be the significant predictor of outcomes. The combination of PERCIST and RECIST would provide clinicians more accurate information of therapeutic response in earlier stage of treatment.
机译:背景:18 F-FDG PET / CT越来越多地用于评估非小细胞肺癌(NSCLC)患者的治疗反应。需要一种准确的标准来评估疗效并预测预后。这项研究的目的是通过比较实体瘤的PET反应标准(PERCIST)与实体肿瘤的反应评估标准(RECIST)在PET / CT上评估NSCLC的治疗反应。方法:对44例接受化疗但未进行手术的非小细胞肺癌患者进行了研究。根据RECIST和PERCIST方法,使用18 F-FDG PET和CT评估化疗反应。在化疗之前和化疗后2或4-6个周期进行了PET / CT扫描。使用配对t检验比较治疗前后肿瘤最长直径和标准化摄取值(SUV)(校正为瘦体重,SUL)的百分比变化。根据RECIST和PERCIST,响应分为4个级别:CR(CMR)= 1,PR(PMR)= 2,SD(SMD)= 3,PD(PMD)= 4。皮尔逊卡方检验用于比较RECIST和PERCIST中四个水平的比例。最后,使用单变量和多变量Cox比例风险回归方法评估了无进展生存期(PFS)与临床病理参数(例如TNM分期,直径变化百分比以及SUL,RECIST和PERCIST结果等)之间的关系。结果:使用配对t检验,直径和SUL之间的百分比变化百分比差异不显着(t = –1.69,P = 0.098)。然而,在40例患者中,SUL差异无统计学意义(t = –3.31,P = 0.002)。通过卡方检验,RECIST和PERCIST之间的评估结果差异不显着(χ2 = 5.008,P = 0.171)。如果RECIST评估排除了无法在CT图像上找到或识别出的新病变,则RECIST和PERCIST之间的差异非常显着(χ2 = 11.759,P = 0.007)。 SUL峰的降低率(%),RECIST和PERCIST结果是单变量Cox分析的重要因素。但是多元Cox比例风险回归分析表明,只有PERCIST是预测DFS的重要因素[风险比(HR),3.20; 95%(CI),1.85-5.54; P <0.001]。结论:PERCIST和RECIST标准具有良好的一致性,PERCIST(或PET)在检测完全缓解(CR)和病情进展方面更为敏感。 PERCIST可能是结果的重要预测指标。 PERCIST和RECIST的结合将为临床医生在治疗早期提供更准确的治疗反应信息。

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