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首页> 外文期刊>Journal of neuro-oncology. >Imaging response criteria for recurrent gliomas treated with bevacizumab: role of diffusion weighted imaging as an imaging biomarker.
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Imaging response criteria for recurrent gliomas treated with bevacizumab: role of diffusion weighted imaging as an imaging biomarker.

机译:贝伐单抗治疗复发性神经胶质瘤的影像学反应标准:弥散加权成像作为影像学生物标志物的作用。

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The purpose of this study was to assess the usefulness of diffusion weighted imaging as an additional imaging biomarker for treatment response in recurrent/progressive malignant gliomas treated with bevacizumab alone or in combination with other chemotherapeutic agents. Twenty patients treated with bevacizumab alone or concurrent chemotherapy were followed up with serial MR imaging. Volume and ADC values of contrast enhancing lesion (CEL(vol), CEL(ADC)) and also of non-enhancing lesion (NEL(vol), NEL(ADC)) were obtained. CEL(vol) showed a progressive decrease in non-progressors with a median percentage change of -73.2% (P = 0.001) as compared to -33.4% for progressors by 1 year/last imaging (P = 0.382). NEL(vol) also showed a decrease in non-progressors on follow up imaging though only significant for 3 months follow up (P = 0.042). In progressors, CEL(vol) and NEL(vol) showed initial decrease followed by slight increase by 1 year/last imaging though not significant (P value of 0.382 and 0.46, respectively). CEL(ADC) and NEL(ADC) in non-progressors did not show any statistically significant change though there was slight trend for positive percent change especially for CEL(ADC) by 1 year/last imaging follow up study (P value of 0.077 and 0.339, respectively). Progressors showed a progressive negative percent change of CEL(ADC) and NEL(ADC). In progressors, NEL(ADC) decreased at 6 weeks (P = 0.054), 3 months (P = 0.023) and 1 year/last (P = 0.078) as compared to baseline study and was also statistically significant as compared to non-progressors at 6 weeks (P = 0.047) and 3 months (P = 0.025). CEL(ADC) and NEL(ADC) appear to follow different trends over time for non-progressors and progressors with a stable to slightly progressive increase in non-progressors and a progressive decrease in progressors, especially early on. These findings suggest that DWI may be used as an additional imaging biomarker for early treatment response.
机译:这项研究的目的是评估弥散加权成像作为单独使用贝伐单抗或与其他化疗药物联合治疗的复发/进行性恶性神经胶质瘤的治疗反应的附加成像生物标志物的有用性。接受贝伐单抗单独治疗或同时进行化疗的20例患者接受了连续MR成像随访。获得对比增强病变(CEL(vol),CEL(ADC))和非增强病变(NEL(vol),NEL(ADC))的体积和ADC值。 CEL(vol)显示非渐进性患者逐渐减少,中位百分比变化为-73.2%(P = 0.001),相比而言,通过1年/最后一次成像,渐进性患者的-33.4%(P = 0.382)。 NEL(vol)在随访影像学中也显示出非进展的减少,尽管仅在3个月的随访中有显着性意义(P = 0.042)。在进展者中,CEL(vol)和NEL(vol)表现出最初的降低,随后在影像学1年/末次影像学上略有增加,尽管并不显着(P值分别为0.382和0.46)。非进展者中的CEL(ADC)和NEL(ADC)没有显示任何统计学上的显着变化,尽管在1年/最后一次影像学随访研究中,尤其是CEL(ADC)的阳性百分比变化有轻微趋势(P值为0.077和分别为0.339)。进阶者显示CEL(ADC)和NEL(ADC)的负百分比逐渐变化。在进展中,与基线研究相比,NEL(ADC)在第6周(P = 0.054),3个月(P = 0.023)和1年/最后(P = 0.078)下降,并且与非进展者相比也具有统计学意义6周(P = 0.047)和3个月(P = 0.025)。对于非进阶者和进阶者,CEL(ADC)和NEL(ADC)随时间变化的趋势似乎有所不同,非进阶者的增长稳定到略有渐进,而进阶者的下降则逐渐,尤其是在早期。这些发现表明,DWI可以用作早期治疗反应的附加成像生物标志物。

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