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氧增强和动态对比增强光声断层扫描提供肿瘤血管功能、缺氧和坏死的替代生物标志物。

Oxygen-Enhanced and Dynamic Contrast-Enhanced Optoacoustic Tomography Provide Surrogate Biomarkers of Tumor Vascular Function, Hypoxia, and Necrosis.

机构信息

Department of Physics, University of Cambridge, Cambridge, United Kingdom.

Cancer Research UK Cambridge Institute, University of Cambridge, Cambridge, United Kingdom.

出版信息

Cancer Res. 2018 Oct 15;78(20):5980-5991. doi: 10.1158/0008-5472.CAN-18-1033. Epub 2018 Aug 16.

DOI:10.1158/0008-5472.CAN-18-1033
PMID:30115696
Abstract

Measuring the functional status of tumor vasculature, including blood flow fluctuations and changes in oxygenation, is important in cancer staging and therapy monitoring. Current clinically approved imaging modalities suffer long procedure times and limited spatiotemporal resolution. Optoacoustic tomography (OT) is an emerging clinical imaging modality that may overcome these challenges. By acquiring data at multiple wavelengths, OT can interrogate hemoglobin concentration and oxygenation directly and resolve contributions from injected contrast agents. In this study, we tested whether two dynamic OT techniques, oxygen-enhanced (OE) and dynamic contrast-enhanced (DCE)-OT, could provide surrogate biomarkers of tumor vascular function, hypoxia, and necrosis. We found that vascular maturity led to changes in vascular function that affected tumor perfusion, modulating the DCE-OT signal. Perfusion in turn regulated oxygen availability, driving the OE-OT signal. In particular, we demonstrate for the first time a strong per-tumor and spatial correlation between imaging biomarkers derived from these techniques and tumor hypoxia quantified Our findings indicate that OT may offer a significant advantage for localized imaging of tumor response to vascular-targeted therapies when compared with existing clinical DCE methods. Imaging biomarkers derived from optoacoustic tomography can be used as surrogate measures of tumor perfusion and hypoxia, potentially yielding rapid, multiparametric, and noninvasive cancer staging and therapeutic response monitoring in the clinic. http://cancerres.aacrjournals.org/content/canres/78/20/5980/F1.large.jpg .

摘要

测量肿瘤血管的功能状态,包括血流波动和氧合变化,在癌症分期和治疗监测中很重要。目前临床批准的成像方式存在程序时间长和空间分辨率有限的问题。光声断层扫描(OT)是一种新兴的临床成像方式,可能克服这些挑战。通过在多个波长采集数据,OT 可以直接询问血红蛋白浓度和氧合,并解析来自注入对比剂的贡献。在这项研究中,我们测试了两种动态 OT 技术,氧增强(OE)和动态对比增强(DCE)-OT,是否可以提供肿瘤血管功能、缺氧和坏死的替代生物标志物。我们发现血管成熟度导致血管功能变化,影响肿瘤灌注,调节 DCE-OT 信号。灌注反过来调节氧气供应,驱动 OE-OT 信号。特别是,我们首次证明了这些技术衍生的成像生物标志物与肿瘤缺氧之间存在强烈的肿瘤内和空间相关性,该相关性是通过定量评估得到的。我们的研究结果表明,与现有的临床 DCE 方法相比,OT 可能为局部成像肿瘤对血管靶向治疗的反应提供显著优势。光声断层扫描衍生的成像生物标志物可作为肿瘤灌注和缺氧的替代指标,有望在临床上实现快速、多参数、无创的癌症分期和治疗反应监测。

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