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基于上转换纳米粒子的全集成超薄术中微型成像仪用于癌症检测

Fully Integrated Ultra-thin Intraoperative Micro-imager for Cancer Detection Using Upconverting Nanoparticles.

机构信息

Department of Electrical Engineering and Computer Sciences, University of California, Berkeley, CA, 94720, USA.

Molecular Foundry, Lawrence Berkeley National Laboratory, Berkeley, CA, 94720, USA.

出版信息

Mol Imaging Biol. 2023 Feb;25(1):168-179. doi: 10.1007/s11307-022-01710-8. Epub 2022 Mar 21.

Abstract

PURPOSE

Intraoperative detection and removal of microscopic residual disease (MRD) remain critical to the outcome of cancer surgeries. Today's minimally invasive surgical procedures require miniaturization and surgical integration of highly sensitive imagers to seamlessly integrate into the modern clinical workflow. However, current intraoperative imagers remain cumbersome and still heavily dependent on large lenses and rigid filters, precluding further miniaturization and integration into surgical tools.

PROCEDURES

We have successfully engineered a chip-scale intraoperative micro-imager array-without optical filters or lenses-integrated with lanthanide-based alloyed upconverting nanoparticles (aUCNPs) to achieve tissue imaging using a single micro-chip. This imaging platform is able to leverage the unique optical properties of aUCNPs (long luminescent lifetime, high-efficiency upconversion, no photobleaching) by utilizing a time-resolved imaging method to acquire images using a 36-by-80-pixel, 2.3 mm [Formula: see text] 4.8 mm silicon-based electronic imager micro-chip, that is, less than 100-µm thin. Each pixel incorporates a novel architecture enabling automated background measurement and cancellation. We have validated the performance, spatial resolution, and the background cancellation scheme of the imaging platform, using resolution test targets and mouse prostate tumor sample intratumorally injected with aUCNPs. To demonstrate the ability to image MRD, or tumor margins, we evaluated the imaging platform in visualizing a single-cell thin section of the injected prostate tumor sample.

RESULTS

Tested on USAF resolution targets, the imager is able to achieve a resolution of 71 µm. We have also demonstrated successful background cancellation, achieving a signal-to-background ratio of 8 when performing ex vivo imaging on aUCNP-injected prostate tumor sample, improved from originally 0.4. The performance of the imaging platform on single-cell layer sections was also evaluated and the sensor achieved a signal-to-background ratio of 4.3 in resolving cell clusters with sizes as low as 200 cells.

CONCLUSION

The imaging system proposed here is a scalable chip-scale ultra-thin alternative for bulky conventional intraoperative imagers. Its novel pixel architecture and background correction scheme enable visualization of microscopic-scale residual disease while remaining completely free of lenses and filters, achieving an ultra-miniaturized form factor-critical for intraoperative settings.

摘要

目的

在癌症手术中,术中检测和清除微观残留疾病(MRD)仍然是至关重要的。如今的微创手术需要微型化和手术集成高度敏感的成像仪,以便无缝集成到现代临床工作流程中。然而,目前的术中成像仪仍然很笨重,仍然严重依赖于大镜头和刚性滤光片,从而无法进一步实现微型化和集成到手术工具中。

过程

我们已经成功地设计了一种没有光学滤波器或透镜的芯片级术中微成像仪阵列,该阵列与镧系合金上转换纳米粒子(aUCNP)集成在一起,以使用单个微芯片实现组织成像。该成像平台能够利用 aUCNP 的独特光学特性(长荧光寿命、高效上转换、无光漂白),通过使用时间分辨成像方法来获取图像,该方法使用 36 乘 80 像素、2.3mm[公式:见正文]4.8mm 硅基电子成像微芯片,即小于 100-µm 厚。每个像素都采用一种新颖的架构,能够实现自动背景测量和消除。我们已经使用分辨率测试目标和在体内注射 aUCNP 的小鼠前列腺肿瘤样本验证了成像平台的性能、空间分辨率和背景消除方案。为了证明检测 MRD 或肿瘤边缘的能力,我们评估了该成像平台在观察注射前列腺肿瘤样本的单细胞薄层中的成像能力。

结果

在 USAF 分辨率测试目标上进行测试时,该成像仪能够实现 71µm 的分辨率。我们还成功地实现了背景消除,在对体内注射 aUCNP 的前列腺肿瘤样本进行离体成像时,实现了 8 的信号与背景比,比最初的 0.4 有所提高。还评估了成像平台在单细胞层切片上的性能,该传感器在分辨低至 200 个细胞的细胞簇时,实现了 4.3 的信号与背景比。

结论

这里提出的成像系统是一种可扩展的芯片级超薄替代方案,替代了笨重的传统术中成像仪。其新颖的像素架构和背景校正方案能够实现微观残留疾病的可视化,同时完全不使用透镜和滤波器,实现了超小型化的外形,这对术中环境至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d82a/9970948/148e77fd80c1/11307_2022_1710_Fig1_HTML.jpg

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