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功能光学相干断层扫描对肿瘤微血管放射生物学反应的临床前纵向成像。

Preclinical longitudinal imaging of tumor microvascular radiobiological response with functional optical coherence tomography.

机构信息

University of Toronto, Department of Medical Biophysics, Toronto, Canada.

University Health Network, Princess Margaret Cancer Centre, Toronto, Canada.

出版信息

Sci Rep. 2018 Jan 8;8(1):38. doi: 10.1038/s41598-017-18635-w.

Abstract

Radiation therapy (RT) is widely used for cancer treatment, alone or in combination with other therapies. Recent RT advances have revived interest in delivering higher dose in fewer fractions, which may invoke both cellular and microvascular damage mechanisms. Microvasculature may thus be a potentially sensitive functional biomarker of RT early response, especially for such emerging RT treatments. However it is difficult to measure directly and non-invasively, and its time course, dose dependencies, and overall importance in tumor control are unclear. We use functional optical coherence tomography for quantitative longitudinal in vivo imaging in preclinical models of human tumor xenografts subjected to 10, 20 and 30 Gy doses, furnishing a detailed assessment of vascular remodeling following RT. Immediate (minutes to tens of minutes) and early (days to weeks) RT responses of microvascular supply, as well as tumor volume and fluorescence intensity, were quantified and demonstrated robust and complex temporal dose-dependent behaviors. The findings were compared to theoretical models proposed in the literature.

摘要

放射治疗(RT)广泛用于癌症的单独或联合治疗。最近的 RT 进展激发了人们对在更少的分次中给予更高剂量的兴趣,这可能会引起细胞和微血管损伤机制。因此,微血管可能是 RT 早期反应的潜在敏感功能生物标志物,特别是对于这种新兴的 RT 治疗。然而,它很难直接和无创地测量,其时间过程、剂量依赖性以及在肿瘤控制中的整体重要性尚不清楚。我们使用功能光学相干断层扫描(functional optical coherence tomography,FOCT)对接受 10、20 和 30Gy 剂量的人肿瘤异种移植的临床前模型进行定量纵向体内成像,详细评估了 RT 后的血管重塑。对微血管供应的即时(数分钟至数十分钟)和早期(数天至数周)RT 反应,以及肿瘤体积和荧光强度进行了量化,并显示出强大而复杂的时间剂量依赖性行为。研究结果与文献中提出的理论模型进行了比较。

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