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首页> 外文期刊>NMR in biomedicine >From single-pulsed field gradient to double-pulsed field gradient MR: gleaning new microstructural information and developing new forms of contrast in MRI
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From single-pulsed field gradient to double-pulsed field gradient MR: gleaning new microstructural information and developing new forms of contrast in MRI

机译:从单脉冲场梯度到双脉冲场梯度MR:在MRI中收集新的微结构信息并开发新的对比形式

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One of the hallmarks of diffusion NMR and MRI is its ability to utilize restricted diffusion to probe compartments much smaller than the excited volume or the MRI voxel, respectively, and to extract microstructural information from them. Single-pulsed field gradient (s-PFG) MR methodologies have been employed with great success to probe microstructures in various disciplines, ranging from chemistry to neuroscience. However, s-PFG MR also suffers from inherent shortcomings, especially when specimens are characterized by orientation or size distributions: in such cases, the microstructural information available from s-PFG experiments is limited or lost. Double-pulsed field gradient (d-PFG) MR methodology, an extension of s-PFG MR, has attracted attention owing to recent theoretical studies predicting that it can overcome certain inherent limitations of s-PFG MR. In this review, we survey the microstructural features that can be obtained from conventional s-PFG methods in the different q regimes, and highlight its limitations. The experimental aspects of d-PFG methodology are then presented, together with an overview of its theoretical underpinnings and a general framework for relating the MR signal decay and material microstructure, affording new microstructural parameters. We then discuss recent studies that have validated the theory using phantoms in which the ground truth is well known a priori, a crucial step prior to the application of d-PFG methodology in neuronal tissue. The experimental findings are in excellent agreement with the theoretical predictions and reveal, inter alia, zero-crossings of the signal decay, robustness towards size distributions and angular dependences of the signal decay from which accurate microstructural parameters, such as compartment size and even shape, can be extracted. Finally, we show some initial findings in d-PFG MR imaging. This review lays the foundation for future studies, in which accurate and novel microstructural information could be extracted from complex biological specimens, eventually leading to new forms of contrast in MRI.
机译:扩散NMR和MRI的标志之一是其利用受限扩散分别探测比激发体积或MRI体素小得多的隔室并从中提取微结构信息的能力。单脉冲场梯度(s-PFG)MR方法已成功应用于探测从化学到神经科学等各个学科的微观结构。但是,s-PFG MR也存在固有的缺陷,特别是当样品具有方向或尺寸分布特征时:在这种情况下,s-PFG实验中可获得的微观结构信息会受到限制或丢失。双脉冲场梯度(d-PFG)MR方法是s-PFG MR的扩展,由于最近的理论研究预测它可以克服s-PFG MR的某些固有局限性而受到关注。在这篇综述中,我们调查了可以在不同的q方案中从常规s-PFG方法获得的微观结构特征,并强调了其局限性。然后介绍了d-PFG方法的实验方面,以及其理论基础的概述以及用于关联MR信号衰减和材料微结构的通用框架,从而提供了新的微结构参数。然后,我们将讨论最近的研究,这些研究已使用幻像验证了该理论,在幻像中,先验先验知识是众所周知的,这是在d-PFG方法应用于神经元组织之前的关键步骤。实验结果与理论预测非常吻合,除其他外,揭示了信号衰减的零交叉,对尺寸分布的鲁棒性以及信号衰减的角度依赖性,从中可以得到精确的微结构参数,例如隔室尺寸和均匀形状,可以提取。最后,我们在d-PFG MR成像中显示了一些初步发现。这篇综述为将来的研究奠定了基础,在该研究中,可以从复杂的生物学标本中提取出准确而新颖的微观结构信息,最终导致MRI出现新的对比形式。

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