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Noninvasive Anatomical and Functional Imaging of Orthotopic Glioblastoma Development and Therapy using Multispectral Optoacoustic Tomography

机译:原位胶质母细胞瘤发展和治疗的无创解剖和功能成像使用多光谱光声层析成像。

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摘要

PURPOSE: Here we demonstrate the potential of multispectral optoacoustic tomography (MSOT), a new non-invasive structural and functional imaging modality, to track the growth and changes in blood oxygen saturation (sO2) in orthotopic glioblastoma (GBMs) and the surrounding brain tissues upon administration of a vascular disruptive agent (VDA). METHODS: Nude mice injected with U87MG tumor cells were longitudinally monitored for the development of orthotopic GBMs up to 15 days and observed for changes in sO2 upon administration of combretastatin A4 phosphate (CA4P, 30 mg/kg), an FDA approved VDA for treating solid tumors. We employed a newly-developed non-negative constrained approach for combined MSOT image reconstruction and unmixing in order to quantitatively map sO2 in whole mouse brains. RESULTS: Upon longitudinal monitoring, tumors could be detected in mouse brains using single-wavelength data as early as 6 days post tumor cell inoculation. Fifteen days post-inoculation, tumors had higher sO2 of 63 ± 11% (n = 5, P < .05) against 48 ± 7% in the corresponding contralateral brain, indicating their hyperoxic status. In a different set of animals, 42 days post-inoculation, tumors had lower sO2 of 42 ± 5% against 49 ± 4% (n = 3, P < .05) in the contralateral side, indicating their hypoxic status. Upon CA4P administration, sO2 in 15 days post-inoculation tumors dropped from 61 ± 9% to 36 ± 1% (n = 4, P < .01) within one hour, then reverted to pre CA4P treatment values (63 ± 6%) and remained constant until the last observation time point of 6 hours. CONCLUSION: With the help of advanced post processing algorithms, MSOT was capable of monitoring the tumor growth and assessing hemodynamic changes upon administration of VDAs in orthotopic GBMs.
机译:目的:在这里我们展示多光谱光声层析成像(MSOT)的潜力,一种新的非侵入性结构和功能成像方式,可以追踪原位胶质母细胞瘤(GBM)和周围脑组织中血氧饱和度(sO2)的增长和变化给予血管破坏剂(VDA)后。方法:对注射了U87MG肿瘤细胞的裸鼠进行长达15天的纵向监测,以观察原位GBM的发生,并观察给予FDA批准的VDA磷酸康维他汀A4(CA4P,30 mg / kg)治疗固体时sO2的变化。肿瘤。我们采用了一种新开发的非负约束方法来组合MSOT图像重建和分解,以便在整个小鼠大脑中定量映射sO2。结果:通过纵向监测,最早在肿瘤细胞接种后6天就可以使用单波长数据在小鼠大脑中检测到肿瘤。接种后15天,肿瘤的sO2较高,为63±11%(n = 5,P <.05),而对侧大脑中的血氧饱和度则为48±7%。在另一组动物中,接种后42天,肿瘤对侧的sO2较低,为42±5%,而对侧则为49±4%(n = 3,P <.05),表明它们处于低氧状态。施用CA4P后,肿瘤接种后15天的sO2在1小时内从61±9%降至36±1%(n = 4,P <.01),然后恢复至CA4P治疗前的数值(63±6%)并保持恒定,直到最后一个观察时间点6小时为止。结论:借助先进的后处理算法,MSOT能够监测原位GBM中VDA给药后的肿瘤生长并评估血液动力学变化。

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