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Quantitative mapping of tumor vascularity using volumetric contrast-enhanced ultrasound.

机译:肿瘤血管基使用体积对比增强超声定量映射。

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摘要

The goal of this research project was to develop a volumetric strategy for real-time monitoring and characterization of tumor blood flow using microbubble contrast agents and ultrasound (US) imaging.Volumetric contrast-enhanced US (VCEUS) imaging was implemented on a SONIX RP US system (Ultrasonix Medical Corp, Richmond, BC) equipped with a broadband 4DL14-5/38 probe. Using a microbubble-sensitive harmonic imaging mode (transducer transmits at 5 MHz and receives at 10 MHz), acquisition of postscan-converted VCEUS data was achieved at a volume rate of 1 Hz. After microbubble infusion, custom data processing software was used to derive microbubble time-intensity curve-specific parameters, namely, blood volume (IPK), transit time (T1/2PK), flow rate (SPK), and tumor perfusion (AUC).Using a preclinical breast cancer animal model, it is shown that millimeter-sized deviations in transducer positioning can have profound implications on US-based blood flow estimators, with errors ranging from 6.4% to 40.3% and dependent on both degree of misalignment (offset) and particular blood flow estimator. These errors indicate that VCEUS imaging should be considered in tumor analyses, because they incorporate the entire mass and not just a representative planar cross-section. After administration of an antiangiogenic therapeutic drug (bevacizumab), tumor growth was significantly retarded compared with control tumors (P > 0.03) and reflects observed changes in VCEUS-based blood flow measurements. Analysis of immunohistologic data revealed no differences in intratumoral necrosis levels (P = 0.70), but a significant difference was found when comparing microvessel density counts in control with therapy group tumors (P = 0.05).VCEUS imaging was shown to be a promising modality for monitoring changes in tumor blood flow. Preliminary experimental results are encouraging, and this imaging modality may prove clinically feasible for detecting and monitoring the early antitumor effects in response to cancer drug therapy.
机译:该研究项目的目标是使用微泡造影剂的实时监测和表征肿瘤血流的实时监测和表征,超声(US)成像。在Sonix RP我们上实施了volumetric对比度增强的美国(Vceus)成像系统(Ultrasonix Medical Corp,Richmond,BC)配备了宽带4DL14-5 / 38探头。使用微泡敏感谐波成像模式(换能器在5MHz处透射并在10MHz处接收),以1 Hz的体积速率获得后架构转换的Vceus数据的获取。微泡输注后,定制数据处理软件用于导出微泡时间强度曲线特异性参数,即血容量(IPK),过渡时间(T1 / 2PK),流速(SPK)和肿瘤灌注(AUC)。使用临床乳腺癌动物模型,表明传感器定位中的毫米尺寸的偏差可以对美国的血流估算器具有深远的影响,误差范围为6.4%至40.3%,依赖于两种未对准(偏移)和特定的血流估算器。这些误差表明蠕动成像应在肿瘤分析中考虑,因为它们包含整个质量,而不仅仅是代表性的平面横截面。在施用抗血管生成治疗药物(Bevacizumab)后,与对照肿瘤相比,肿瘤生长显着延迟(P> 0.03),并反映了观察到基于Vceus的血流测量的变化。免疫组织数据的分析显示肿瘤坏死水平没有差异(p = 0.70),但在将微血管密度计数与治疗组肿瘤的对照中进行比较时发现显着差异(P = 0.05).VCEUS成像被证明是一个有希望的模态监测肿瘤血流的变化。初步实验结果是令人抱怨的,这种成像模态可以证明临床上可行的可行,用于检测和监测癌症药物治疗的早期抗肿瘤效应。

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