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基于微线圈的 MR 相位成像和锰增强显微镜,直接光学关联胶质肿瘤神经球。

Microcoil-based MR phase imaging and manganese enhanced microscopy of glial tumor neurospheres with direct optical correlation.

机构信息

Department of Radiology, Medical Physics, University Medical Center, Freiburg, Germany.

出版信息

Magn Reson Med. 2012 Jul;68(1):86-97. doi: 10.1002/mrm.23208. Epub 2011 Nov 29.

Abstract

Susceptibility differences among tissues were recently used for highlighting complementary contrast in MRI different from the conventional T(1), T(2), or spin density contrasts. This method, based on the signal phase, previously showed improved image contrast of human or rodent neuroarchitecture in vivo, although direct MR phase imaging of cellular architecture was not available until recently. In this study, we present for the first time the ability of microcoil-based phase MRI to resolve the structure of human glioma neurospheres at significantly improved resolutions (10 × 10 μm(2)) with direct optical image correlation. The manganese chloride property to function as a T(1) contrast agent enabled a closer examination of cell physiology with MRI. Specifically the temporal changes of manganese chloride uptake, retention and release time within and from individual clusters were assessed. The optimal manganese chloride concentration for improved MR signal enhancement was determined while keeping the cellular viability unaffected. The presented results demonstrate the possibilities to reveal structural and functional observation of living glioblastoma human-derived cells. This was achieved through the combination of highly sensitive microcoils, high magnetic field, and methods designed to maximize contrast to noise ratio. The presented approach may provide a powerful multimodal tool that merges structural and functional information of submilimeter biological samples.

摘要

组织间的敏感性差异最近被用于突出 MRI 中的对比,这种对比与传统的 T(1)、T(2)或自旋密度对比不同。这种基于信号相位的方法以前曾显示出改善了人体或啮齿动物神经结构的体内图像对比度,尽管直到最近才能够直接进行细胞结构的磁共振相位成像。在这项研究中,我们首次展示了微线圈相位 MRI 的能力,该技术能够以显著提高的分辨率(10×10μm²)解析人神经球的结构,并且可以直接与光学图像相关联。氯化锰作为 T(1)对比剂的特性使我们能够更仔细地用 MRI 检查细胞生理学。具体而言,评估了锰盐在单个簇内和从单个簇中摄取、保留和释放时间的时间变化。在不影响细胞活力的情况下,确定了最佳的锰盐浓度以提高 MR 信号增强。所呈现的结果表明了揭示活的神经胶质瘤衍生细胞的结构和功能观察的可能性。这是通过结合高灵敏度微线圈、高磁场以及旨在最大化对比噪声比的方法来实现的。所提出的方法可以提供一种强大的多模态工具,该工具融合了亚毫米级生物样本的结构和功能信息。

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