论文标题

切片选择性零回波时间成像,基于自旋锁

Slice-selective Zero Echo Time imaging of ultra-short T2 tissues based on spin-locking

论文作者

Borreguero, J., Galve, F., Algarín, J. M., Benlloch, J. M., Alonso, J.

论文摘要

目的:使用适合体内最短的组织的切片选择方法扩展零回波时间(ZTE)脉冲序列的功能。 方法:我们引入了两个新序列,它们将自旋锁定脉冲集成到标准的ZTE成像中以实现切片选择:一个用于中等短$ T_2 $(不喜欢),另一个用于超短$ T_2 $样本(Preslop)。这些方法利用较慢的信号衰减(在$ t_ {1ρ} \ gg t_2 $)中保留在选择过程中的切片中的磁化,否则该磁化值与$ T_2 $相当或什至更长。 结果:我们证明了对2D成像的切片轮廓和位置的控制。我们测量自旋锁定期间的磁化衰减时间($ t_ {1ρ} $)作为脉冲振幅的函数,显示出低至10 UT的振幅的显着寿命增强。我们显示了切成薄片的样品的成像,其中$ t_2 $的特征时间在单一毫秒范围内,不喜欢和前圈,而后者则用于subilsecond $ t_2 $ thispues。与标准的3D中兴序列相比,Preslop在较短的扫描时间中达到了相同的信噪比(SNR),我们认为这是由于有限间隙的填充方案在$ K $ - 空间中心的填充方案造成的,该中心是$ K $ - 空间不可避免的ZTE序列的填充方案。最后,我们讨论了不喜欢的组合与动态脱钩序列,以避免这种中心差距,从而导致进一步的扫描时间加速。 结论:所提出的序列能够将$ t_2 $ $ t_2 $的组织切成序列的2D成像,低至275 US,在临床上可接受的扫描时间内具有良好的SNR。

Purpose: To expand the capabilities of Zero Echo Time (ZTE) pulse sequences with a slice selection method suitable for the shortest-lived tissues in the body. Methods: We introduce two new sequences that integrate spin-locking pulses into standard ZTE imaging to achieve slice selection: one for moderately short $T_2$ (DiSLoP), the other for ultra-short $T_2$ samples (PreSLoP). These methods exploit the slower signal decay (at $T_{1ρ}\gg T_2$) to retain the magnetization in the slices during the selection process, which is otherwise comparable to or even much longer than $T_2$. Results: We demonstrate control over the slice profiles and positions for 2D imaging. We measure magnetization decay times during spin-locking ($T_{1ρ}$) as a function of pulse amplitude, showing significant lifetime enhancement for amplitudes as low as 10 uT. We show imaging of slice-selected samples with $T_2$ characteristic times in the range of single milliseconds with DiSLoP and PreSLoP, and with the latter for sub-millisecond $T_2$ tissues. As compared to standard 3D ZTE sequences, PreSLoP achieves the same signal-to-noise ratio (SNR) in 2-5 times shorter scan times, and we argue that this is due to the filling scheme of the finite gap at the center of $k$-space unavoidable with ZTE sequences. Finally, we discuss a combination of DiSLoP with a dynamical decoupling sequence to avoid this central gap, leading to further scan time accelerations. Conclusions: The proposed sequences are capable of slice-selected 2D imaging of tissues with $T_2$ as low as 275 us with good SNR within clinically acceptable scan times.

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