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亲脂性染料兼容的脑透明化技术,可在胶质母细胞瘤大鼠模型中进行磁共振/高分辨率荧光成像的相关研究。

Lipophilic dye-compatible brain clearing technique allowing correlative magnetic resonance/high-resolution fluorescence imaging in rat models of glioblastoma.

机构信息

Gene Therapy Program, Dana-Farber/Boston Children's Centre for Cancer and Blood Disorders, Boston, MA, USA.

Harvard Medical School, Boston, MA, USA.

出版信息

Sci Rep. 2020 Oct 21;10(1):17974. doi: 10.1038/s41598-020-75137-y.

Abstract

In this work we optimized a novel approach for combining in vivo MRI and ex vivo high-resolution fluorescence microscopy that involves: (i) a method for slicing rat brain tissue into sections with the same thickness and spatial orientation as in in vivo MRI, to better correlate in vivo MRI analyses with ex-vivo imaging via scanning confocal microscope and (ii) an improved clearing protocol compatible with lipophilic dyes that highlight the neurovascular network, to obtain high tissue transparency while preserving tissue staining and morphology with no significant tissue shrinkage or expansion. We applied this methodology in two rat models of glioblastoma (GBM; U87 human glioma cells and patient-derived human glioblastoma cancer stem cells) to demonstrate how vital the information retrieved from the correlation between MRI and confocal images is and to highlight how the increased invasiveness of xenografts derived from cancer stem cells may not be clearly detected by standard in vivo MRI approaches. The protocol studied in this work could be implemented in pre-clinical GBM research to further the development and validation of more predictive and translatable MR imaging protocols that can be used as critical diagnostic and prognostic tools. The development of this protocol is part of the quest for more efficacious treatment approaches for this devastating and still uncurable disease. In particular, this approach could be instrumental in validating novel MRI-based techniques to assess cellular infiltration beyond the macroscopic tumor margins and to quantify neo-angiogenesis.

摘要

在这项工作中,我们优化了一种将体内 MRI 和离体高分辨率荧光显微镜结合的新方法,包括:(i)一种将大鼠脑组织切成与体内 MRI 相同厚度和空间方向的切片的方法,以便通过扫描共聚焦显微镜更好地将体内 MRI 分析与离体成像相关联,(ii)一种与亲脂性染料兼容的改进的透明化方案,突出神经血管网络,以获得高组织透明度,同时保持组织染色和形态,无明显的组织收缩或扩张。我们将这种方法应用于两种胶质母细胞瘤(GBM;U87 人神经胶质瘤细胞和患者来源的人胶质母细胞瘤癌症干细胞)的大鼠模型中,以证明从 MRI 和共聚焦图像之间的相关性中获取的信息是多么重要,并强调源自癌症干细胞的异种移植物的侵袭性增加可能无法通过标准的体内 MRI 方法清楚地检测到。本研究中所研究的方案可以在 GBM 的临床前研究中实施,以进一步开发和验证更具预测性和可转化的 MRI 成像方案,这些方案可作为关键的诊断和预后工具。该方案的开发是寻求更有效的治疗方法来治疗这种破坏性且仍然无法治愈的疾病的一部分。特别是,这种方法对于验证基于 MRI 的新技术来评估宏观肿瘤边缘以外的细胞浸润和量化新生血管形成非常重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d81/7578790/fe26a2528cdf/41598_2020_75137_Fig1_HTML.jpg

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