Ultrafast Power Doppler Ultrasound Enables Longitudinal Tracking of Vascular Changes that Correlate with Immune Response After Radiotherapy.

Shannon E Martello, Jixin Xia, Jiro Kusunose, Benjamin C Hacker, McKenzie A Mayeaux, Erica J Lin, Adrienne Hawkes, Aparna Singh, Charles F Caskey, Marjan Rafat
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Abstract

Background: While immunotherapy shows great promise in patients with triple negative breast cancer, many will not respond to treatment. Radiotherapy has the potential to prime the tumor-immune microenvironment for immunotherapy. However, predicting response is difficult due to tumor heterogeneity across patients, which necessitates personalized medicine strategies that incorporate tumor tracking into the therapeutic approach. Here, we investigated the use of ultrasound (US) imaging of the tumor vasculature to monitor the tumor response to treatment.

Methods: We utilized ultrafast power doppler US to track the vascular response to radiotherapy over time. We used 4T1 (metastatic) and 67NR (non-metastatic) breast cancer models to determine if US measurements corroborate conventional immunostaining analysis of the tumor vasculature. To evaluate the effects of radiation, tumor volume and vascular index were calculated using US, and the correlation between vascular changes and immune cell infiltration was determined.

Results: US tumor measurements and the quantified vascular response to radiation were confirmed with caliper measurements and immunostaining, respectively, demonstrating a proof-of-principle method for non-invasive vascular monitoring. Additionally, we found significant infiltration of CD8 + T cells into irradiated tumors 10 days after radiation, which followed a sustained decline in vascular index and an increase in splenic CD8 + T cells that was first observed 1 day post-radiation.

Conclusions: Our findings reveal that ultrafast power doppler US can evaluate changes in tumor vasculature that are indicative of shifts in the tumor-immune microenvironment. This work may lead to improved patient outcomes through observing and predicting response to therapy.

超声成像可纵向追踪放疗后与免疫反应相关的血管变化
背景:虽然免疫疗法在三阴性乳腺癌患者中大有可为,但许多患者对治疗无效。放疗有可能为免疫疗法提供肿瘤免疫微环境。然而,由于不同患者的肿瘤具有异质性,因此很难预测反应,这就需要将肿瘤追踪纳入治疗方法的个性化医疗策略。在此,我们研究了利用肿瘤血管的超声(US)成像来监测肿瘤对治疗的反应:方法:我们利用超快功率多普勒超声来纵向追踪血管对放疗的反应。我们使用 4T1(转移性)和 67NR(非转移性)乳腺癌模型来确定 US 测量是否与肿瘤血管的传统组织学分析相吻合。为了评估辐射的影响,我们用 US 计算了肿瘤体积和血管指数,并确定了血管变化与免疫细胞浸润之间的相关性:结果:US 测量的肿瘤体积和量化的血管对辐射的反应分别得到了卡尺测量和免疫组化染色的证实,证明这是一种非侵入性血管监测的原理性方法。此外,我们发现 CD8 + T 细胞在辐射 10 天后明显浸润到受辐射的肿瘤中,随后血管指数持续下降,脾脏 CD8 + T 细胞增加,这在辐射 1 天后首次观察到:我们的研究结果表明,超快功率多普勒 US 可以评估肿瘤血管的变化,这些变化表明肿瘤免疫微环境发生了变化。这项工作可通过观察和预测对治疗的反应来改善患者的预后。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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