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Biomolecular MRI Reporters: evolution of new mechanisms

机译:生物分子MRI记者:新机制的演变

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摘要

Magnetic resonance imaging (MRI) is a powerful technique for observing the function of specific cells and molecules inside living organisms. However, compared to optical microscopy, in which fluorescent protein reporters are available to visualize hundreds of cellular functions ranging from gene expression and chemical signaling to biomechanics, to date relatively few such reporters are available for MRI. Efforts to develop MRI-detectable biomolecules have mainly focused on proteins containing or transporting paramagnetic metals for T1 and T2 relaxation enhancement or large numbers of exchangeable protons for chemical exchange saturation transfer. While these pioneering developments established several key uses of biomolecular MRI, such as imaging of gene expression and functional biosensing, they also revealed that low molecular sensitivity poses a major challenge for broader adoption in biology and medicine. Recently, new classes of biomolecular reporters have been developed based on alternative contrast mechanisms, including enhancement of spin diffusivity, interactions with hyperpolarized nuclei, and modulation of blood flow. These novel reporters promise to improve sensitivity and enable new forms of multiplexed and functional imaging.
机译:磁共振成像(MRI)是一种强大的技术,可用于观察生物体内特定细胞和分子的功能。然而,与光学显微镜相比,荧光蛋白报告基因可用于可视化数百种细胞功能,从基因表达,化学信号传导到生物力学,迄今为止,此类报告基因可用于MRI的情况相对较少。开发MRI可检测的生物分子的努力主要集中在含有或转运顺磁性金属以增强T1和T2弛豫的蛋白质或大量可交换质子用于化学交换饱和转移的蛋白质上。这些开拓性的发展确立了生物分子MRI的几种关键用途,例如基因表达的成像和功能性生物传感,但它们也揭示了低分子敏感性对生物学和医学的广泛采用提出了重大挑战。近来,基于替代的对比机制,已经开发出新的生物分子报告物类别,包括增强自旋扩散性,与超极化核的相互作用以及血流的调节。这些新颖的报道者承诺将提高灵敏度并实现新形式的多路复用和功能成像。

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