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在体内,通过实时超声引导光声成像对光疗期间的异质氧利用进行在线无标记监测。

In vivo, online label-free monitoring of heterogenous oxygen utilization during phototherapy with real-time ultrasound-guided photoacoustic imaging.

作者信息

Langley Andrew, Sweeney Allison, Shethia Ronak T, Bednarke Brooke, Wulandana Faizah, Xavierselvan Marvin, Mallidi Srivalleesha

机构信息

Department of Biomedical Engineering, Tufts University, MA, USA.

出版信息

bioRxiv. 2024 Dec 3:2024.11.27.625759. doi: 10.1101/2024.11.27.625759.

Abstract

Understanding the tumor microenvironment, particularly the vascular density and the availability of oxygen, is key in individualizing treatment approaches and determining their efficacy. While there are many therapies including radiotherapy that are ineffective in hypoxic tumor microenvironments, here we demonstrate the heterogeneous oxygen consumption during photodynamic therapy (PDT), a non-invasive treatment method using localized light to activate a photosensitive drug in the presence of oxygen that has shown high effectiveness in the treatment of various types of tumors, including those presented in head and neck cancer (HNC) patients. While our previous work has demonstrated that blood oxygen saturation (StO) mapped before and after treatment with ultrasound-guided photoacoustic imaging (US-PAI) can be used as a surrogate marker for the regionalized long-term efficacy of PDT, real-time monitoring of StO during PDT could provide additional insights on oxygen consumption and inform dose design for "on the spot" treatment decisions. Specifically, in this work, we integrated the US-PAI transducer probe with PDT light delivery fibers. We tested the setup on murine tumor models intravenously injected with liposomal benzoporphyrin derivative (BPD) photosensitizer at 0.5 mg/kg dose and photodynamic illumination at 100 and 400 mW/cm fluence rate. As expected, we observed with our US-PAI StO images that the rate of oxygen utilization increases when using a high fluence rate (HFR) light dose. Particularly in the higher fluence rate group, we observed StO reaching a minimum mid-light dose, followed by some degree of reoxygenation. US-PAI added the advantage of spatial information to StO monitoring, which allowed us to match regions of re-oxygenation during therapy to retained vascular function with immunohistochemistry. Overall, our results have demonstrated the potential of US-PAI for applications in online dosimetry for cancer therapies such as PDT, using oxygen changes to detect regionalized physiological vascular response in the tumor microenvironment.

摘要

了解肿瘤微环境,尤其是血管密度和氧气供应情况,对于个性化治疗方案及确定其疗效至关重要。虽然包括放疗在内的许多疗法在缺氧肿瘤微环境中无效,但在此我们证明了光动力疗法(PDT)期间的异质氧消耗情况。PDT是一种非侵入性治疗方法,利用局部光照在有氧存在的情况下激活光敏药物,已显示出对包括头颈癌(HNC)患者所患肿瘤在内的各种类型肿瘤具有高效治疗效果。虽然我们之前的工作表明,超声引导光声成像(US-PAI)在治疗前后绘制的血氧饱和度(StO)可用作PDT区域长期疗效的替代标志物,但在PDT期间对StO进行实时监测可为氧消耗提供更多见解,并为“现场”治疗决策的剂量设计提供参考。具体而言,在这项工作中,我们将US-PAI换能器探头与PDT光传输纤维集成在一起。我们在以0.5mg/kg剂量静脉注射脂质体苯卟啉衍生物(BPD)光敏剂并以100和400mW/cm²的光通量率进行光动力照射的小鼠肿瘤模型上测试了该装置。正如预期的那样,通过我们的US-PAI StO图像观察到,使用高光通量率(HFR)光剂量时氧利用率会增加。特别是在高光通量率组中,我们观察到StO在光剂量达到最小值时出现,随后有一定程度的再氧合。US-PAI为StO监测增加了空间信息优势,这使我们能够通过免疫组织化学将治疗期间的再氧合区域与保留的血管功能相匹配。总体而言,我们的结果证明了US-PAI在癌症治疗(如PDT)的在线剂量测定中的应用潜力,即利用氧变化来检测肿瘤微环境中的区域化生理血管反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a536/11642742/cf719f1edea9/nihpp-2024.11.27.625759v1-f0001.jpg

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