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Prediction of Tumor Recurrence and Therapy Monitoring Using Ultrasound-Guided Photoacoustic Imaging

机译:超声引导下的光声成像对肿瘤复发的预测和治疗监测

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摘要

Selection and design of individualized treatments remains a key goal in cancer therapeutics; prediction of response and tumor recurrence following a given therapy provides a basis for subsequent personalized treatment design. We demonstrate an approach towards this goal with the example of photodynamic therapy (PDT) as the treatment modality and photoacoustic imaging (PAI) as a non-invasive, response and disease recurrence monitor in a murine model of glioblastoma (GBM). PDT is a photochemistry-based, clinically-used technique that consumes oxygen to generate cytotoxic species, thus causing changes in blood oxygen saturation (StO2). We hypothesize that this change in StO2 can be a surrogate marker for predicting treatment efficacy and tumor recurrence. PAI is a technique that can provide a 3D atlas of tumor StO2 by measuring oxygenated and deoxygenated hemoglobin. We demonstrate that tumors responding to PDT undergo approximately 85% change in StO2 by 24-hrs post-therapy while there is no significant change in StO2 values in the non-responding group. Furthermore, the 3D tumor StO2 maps predicted whether a tumor was likely to regrow at a later time point post-therapy. Information on the likelihood of tumor regrowth that normally would have been available only upon actual regrowth (10-30 days post treatment) in a xenograft tumor model, was available within 24-hrs of treatment using PAI, thus making early intervention a possibility. Given the advances and push towards availability of PAI in the clinical settings, the results of this study encourage applicability of PAI as an important step to guide and monitor therapies (e.g. PDT, radiation, anti-angiogenic) involving a change in StO2.
机译:选择和设计个性化治疗仍然是癌症治疗的主要目标。给定治疗后反应和肿瘤复发的预测为后续个性化治疗设计提供了基础。我们以胶体母细胞瘤(GBM)鼠模型中的光动力疗法(PDT)作为治疗方式和光声成像(PAI)作为非侵入性,反应和疾病复发监测器的实例证明了实现该目标的方法。 PDT是一种基于光化学的,临床上使用的技术,该技术消耗氧气以产生细胞毒性物质,从而导致血氧饱和度(StO2)发生变化。我们假设StO2的这种变化可能是预测治疗效果和肿瘤复发的替代指标。 PAI是一项可以通过测量氧化和脱氧血红蛋白来提供3D肿瘤StO2图集的技术。我们证明对PDT有反应的肿瘤在治疗后24小时经历StO2约85%的变化,而在无反应组中StO2值没有显着变化。此外,3D肿瘤StO2映射预测了肿瘤在治疗后的某个时间点是否可能长大。通常在异种移植肿瘤模型中只有在实际再生时(治疗后10-30天)才能获得的有关肿瘤再生可能性的信息,在使用PAI的治疗后24小时内即可获得,因此使早期干预成为可能。考虑到PAI在临床环境中的进步并推动了PAI的可用性,这项研究的结果鼓励了PAI的应用,作为指导和监测涉及StO2变化的疗法(例如PDT,放射线,抗血管生成)的重要步骤。

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