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首页> 外文期刊>Advances in Experimental Medicine and Biology >Radiation oxygen biology with pulse electron paramagnetic resonance imaging in animal tumors
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Radiation oxygen biology with pulse electron paramagnetic resonance imaging in animal tumors

机译:脉冲电子顺磁共振成像在动物肿瘤中的放射氧生物学

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摘要

The reduced oxygen in tumors (hypoxia) generates radiation resistance and limits tumor control probability (TCP) at radiation doses without significant normal tissue complication. Modern radiation therapy delivery with intensity-modulated radiation therapy (IMRT) enables complex, high-dose gradient patterns, which avoid sensitive human tissues and organs. EPR oxygen images may allow selection of more resistant parts of a tumor to which to deliver more radiation dose to enhance TCP. EPR O2 images are obtained using injected narrow-line, low relaxation rate trityl spin probes that enable pulse radiofrequency EPR O2 images of tumors in the legs of mice, rats, and rabbits, the latter exceeding 4 cm in size. Low relaxation rates of trityls have enabled novel T1-, rather than T2-, based oximetry, which provides near absolute pO2 imaging. Tomographic image formation and filtered back projection reconstruction are used to generate these images with fixed, linear stepped gradients. Images obtained both with T2 and T1 oximetric images have demonstrated the complex in vivo mechanism explaining the unexpected efficacy of TNFerade, a radiation-inducible adenoviral construct to locally produce TNF-induced vascular as well as radiation damage [1, 2]. The unexpected efficacy of large-dose radiation fractions is seen to be due to an interaction between host microvasculature and tumor cells producing a prompt (15 min) postradiation hypoxia, paralyzing tumor cell repair, and sensitizing tumors. Finally, cure of tumors treated to a single 50 % control dose shows a significant dependence on EPR O2 image hypoxic fractions, best shown with the fraction of voxels less than 10 Torr (HF10). We show that these O2 images provide a quantitative basis for measuring tumor and normal tissue response to abnormally low O2 levels. Measurements of vascular endothelial growth factor (VEGF) production in a specific syngeneic mouse fibrosarcoma, FSa versus fraction of tissue voxels with pO2 less than 10 Torr, produced a slope of 0.14 pg VEGF protein/mg total protein/% HF10. We argue that this quantification may be diagnostic of tumor versus normal tissue, and it may be etiologic in the development of malignancy.
机译:肿瘤中的氧气减少(缺氧)会产生辐射抵抗力,并在没有明显正常组织并发症的情况下限制辐射剂量下的肿瘤控制概率(TCP)。具有强度调制放射疗法(IMRT)的现代放射疗法实现了复杂的高剂量梯度模式,避免了敏感的人体组织和器官。 EPR氧气图像可允许选择肿瘤的更多耐药部位,向其输送更多的辐射剂量以增强TCP。 EPR O2图像是使用注入的窄线,低弛豫速率的三苯甲基自旋探针获得的,该探针可对小鼠,大鼠和兔子的腿部肿瘤进行脉冲射频EPR O2图像,后者的大小超过4厘米。三苯乙稀的低松弛速率已使基于T1而非基于T2的血氧测定法得以实现,它提供了近乎绝对的pO2成像。断层扫描图像形成和滤波后的反投影重建用于生成具有固定线性步进梯度的这些图像。用T2和T1血氧饱和度图像获得的图像已经证明了复杂的体内机制,这说明了TNFerade的出乎意料的功效,TNFerade是一种辐射诱导型腺病毒构建体,可局部产生TNF诱导的血管以及辐射损伤[1、2]。大剂量放射部分的出乎意料的功效被认为是由于宿主微脉管系统与肿瘤细胞之间的相互作用,导致放射后缺氧迅速(15分钟),使肿瘤细胞修复麻痹,并使肿瘤致敏。最后,以单一50%对照剂量治疗的肿瘤的治愈显示出对EPR O2图像缺氧分数的显着依赖性,最好是体素分数小于10 Torr(HF10)的情况最佳。我们显示这些氧气图像为测量肿瘤和正常组织对异常低氧气水平的反应提供了定量基础。测量特定同系小鼠纤维肉瘤中的血管内皮生长因子(VEGF)相对于pO2小于10 Torr的组织体素的比例,产生0.14 pg VEGF蛋白/ mg总蛋白/%HF10的斜率。我们认为,这种量化可能是肿瘤对正常组织的诊断,并且可能是恶性肿瘤发展的病因。

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