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Optical clearing for photoacoustic lympho- and angiography beyond conventional depth limit in vivo

机译:光声淋巴和血管造影的光学清除超出了体内的常规深度限制

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摘要

Photoacoustic (PA) imaging (PAI) is an emerging powerful tool for noninvasive real-time mapping of blood and lymphatic vessels and lymph nodes to diagnose cancer, lymphedema and other diseases. Among different PAI instruments, commercially available raster-scanning optoacoustic mesoscopy (RSOM) (iThera Medical GmbH., Germany) is useful for high-resolution imaging of different tissues with high potential of clinical translation. However, skin light scattering prevents mapping vessels and nodes deeper than 1–2 mm, that limits diagnostic values of PAI including RSOM. Here we demonstrate that glycerol-based tissue optical clearing (TOC) overcomes this challenge by reducing light scattering that improves RSOM depth penetration. In preclinical model of mouse limb , the replacement of conventional acoustic coupling agents such as water on the mixture of 70 % glycerol and 30 % ultrasound (US) gel resulted in the increase of tissue imaging depth in 1.5–2 times with 3D visualization of vessels with diameter down to 20 μm. To distinguish blood and lymphatic networks, we integrated label-free PA angiography ( , imaging of blood vessels), which uses hemoglobin as endogenous contrast agent, with PA lymphography based on labeling of lymphatic vessels with exogenous PA contrast agents. Similar to well-established clinical lymphography, contrast agents were injected in tissue and taken up by lymphatic vessels within a few minutes that provided quick RSOM lymphography. Furthermore, co-injection of PA contrast dye and multilayer nanocomposites as potential low-toxic drug-cargo showed selective prolonged accumulation of nanocomposites in sentinel lymph nodes. Overall, our findings open perspectives for deep and high resolution 3D PA angio- and lymphography, and for PA-guided lymphatic drug delivery using new RSOM & TOC approach.
机译:光声(PA)成像(PAI)是一种新兴的强大工具,可用于对血液和淋巴管以及淋巴结进行无创实时成像,以诊断癌症,淋巴水肿和其他疾病。在不同的PAI仪器中,可商购的光栅扫描光声显微术(RSOM)(iThera Medical GmbH。,德国)可用于对不同组织进行高分辨率成像,并具有很高的临床翻译潜力。但是,皮肤光散射会阻止绘制比1–2mm更深的血管和结点,这限制了包括RSOM在内的PAI的诊断价值。在这里,我们证明了基于甘油的组织光学清除(TOC)通过减少可提高RSOM深度穿透力的光散射克服了这一挑战。在小鼠肢体的临床前模型中,用70%甘油和30%超声(US)凝胶的混合物代替常规的声耦合剂(例如水),可通过3D血管可视化使组织成像深度增加1.5–2倍直径低至20μm。为了区分血液和淋巴网络,我们将使用血红蛋白作为内源性造影剂的无标记PA血管造影(血管成像)与基于外源PA造影剂标记淋巴管的PA淋巴造影相结合。类似于成熟的临床淋巴造影,造影剂被注射到组织中,并在几分钟内被淋巴管吸收,从而提供快速的RSOM淋巴造影。此外,PA对比染料和多层纳米复合材料作为潜在的低毒药物的共同注射显示出纳米复合材料在前哨淋巴结中选择性的长期累积。总体而言,我们的发现为深层和高分辨率3D PA血管造影和淋巴造影术以及使用新的RSOM&TOC方法进行PA引导的淋巴药物递送开辟了前景。

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