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利用梯度调制低功率绝热脉冲通过旋转框架磁共振弛豫对水池和分子动力学进行全脑图谱绘制。

Whole brain mapping of water pools and molecular dynamics with rotating frame MR relaxation using gradient modulated low-power adiabatic pulses.

作者信息

Andronesi Ovidiu C, Bhat Himanshu, Reuter Martin, Mukherjee Shreya, Caravan Peter, Rosen Bruce R

机构信息

Athinoula A. Martinos Center for Biomedical Imaging, Department of Radiology, Massachusetts General Hospital, Harvard Medical School, Boston, MA 02114, USA.

Siemens Medical Solutions USA Inc, Charlestown, MA 02129, USA.

出版信息

Neuroimage. 2014 Apr 1;89:92-109. doi: 10.1016/j.neuroimage.2013.12.007. Epub 2013 Dec 15.

Abstract

Nuclear magnetic resonance (NMR) relaxation in the rotating frame is sensitive to molecular dynamics on the time scale of water molecules interacting with macromolecules or supramolecular complexes, such as proteins, myelin and cell membranes. Hence, longitudinal (T1ρ) and transverse (T2ρ) relaxation in the rotating frame may have a great potential to probe the macromolecular fraction of tissues. This stimulated a large interest in using this MR contrast to image brain under healthy and disease conditions. However, experimental challenges related to the use of intense radiofrequency irradiation have limited the widespread use of T1ρ and T2ρ imaging. Here, we present methodological development to acquire 3D high-resolution or 2D (multi-)slice selective T1ρ and T2ρ maps of the entire human brain within short acquisition times. These improvements are based on a class of gradient modulated adiabatic pulses that reduce the power deposition, provide slice selection, and mitigate artifacts resulting from inhomogeneities of B1 and B0 magnetic fields. Based on an analytical model of the T1ρ and T2ρ relaxation we compute the maps of macromolecular bound water fraction, correlation and exchange time constants as quantitative biomarkers informative of tissue macromolecular content. Results obtained from simulations, phantoms and five healthy subjects are included.

摘要

旋转坐标系中的核磁共振(NMR)弛豫对水分子与大分子或超分子复合物(如蛋白质、髓鞘和细胞膜)相互作用的时间尺度上的分子动力学敏感。因此,旋转坐标系中的纵向(T1ρ)和横向(T2ρ)弛豫在探测组织的大分子部分方面可能具有很大潜力。这激发了人们对在健康和疾病状态下使用这种磁共振对比成像大脑的浓厚兴趣。然而,与使用强射频辐射相关的实验挑战限制了T1ρ和T2ρ成像的广泛应用。在此,我们展示了在短采集时间内获取全脑3D高分辨率或2D(多)切片选择性T1ρ和T2ρ图谱的方法学进展。这些改进基于一类梯度调制绝热脉冲,可降低功率沉积、提供切片选择并减轻由B1和B0磁场不均匀性导致的伪影。基于T1ρ和T2ρ弛豫的解析模型,我们计算大分子结合水分数、相关和交换时间常数的图谱,作为反映组织大分子含量的定量生物标志物。文中包含了模拟、体模和五名健康受试者的结果。

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