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使用FOCI-LASER和多量子滤波器进行单次单体素乳酸测量。

Single-shot single-voxel lactate measurements using FOCI-LASER and a multiple-quantum filter.

作者信息

Payne Geoffrey S, deSouza Nandita M, Messiou Christina, Leach Martin O

机构信息

Cancer Research UK Cancer Imaging Centre, Royal Marsden Hospital and Institute of Cancer Research, Sutton, Surrey, UK.

出版信息

NMR Biomed. 2015 Apr;28(4):496-504. doi: 10.1002/nbm.3276.

Abstract

Measurement of tissue lactate using (1) H MRS is often confounded by overlap with intense lipid signals at 1.3 ppm. Single-voxel localization using PRESS is also compromised by the large chemical shift displacement between voxels for the 4.1 ppm (-CH) resonance and the 1.3 ppm -CH3 resonance, leading to subvoxels with signals of opposite phase and hence partial signal cancellation. To reduce the chemical shift displacement to negligible proportions, a modified semi-LASER sequence was written ("FOCI-LASER", abbreviated as fLASER) using FOCI pulses to permit high RF bandwidth even with the limited RF amplitude characteristic of clinical MRI scanners. A further modification, MQF-fLASER, includes a selective multiple-quantum filter to detect lactate and reject lipid signals. The sequences were implemented on a Philips 3 T Achieva TX system. In a solution of brain metabolites fLASER lactate signals were 2.7 times those of PRESS. MQF-fLASER lactate was 47% of fLASER (the theoretical maximum is 50%) but still larger than PRESS lactate. In oil, the main 1.3 ppm lipid peak was suppressed to less than 1%. Enhanced suppression was possible using increased gradient durations. The minimum detectable lactate concentration was approximately 0.5 mM. Coherence selection gradients needed to be at the magic angle to avoid large water signals derived from intermolecular multiple-quantum coherences. In pilot patient measurements, lactate peaks were often observed in brain tumours, but not in cervix tumours; lipids were effectively suppressed. In summary, compared with PRESS, the fLASER sequence yields greatly superior sensitivity for direct detection of lactate (and equivalent sensitivity for other metabolites), while the single-voxel single-shot MQF-fLASER sequence surpasses PRESS for lactate detection while eliminating substantial signals from lipids. This sequence will increase the potential for in vivo lactate measurement as a biomarker in targeted anti-cancer treatments as well as in measurements of tissue hypoxia.

摘要

使用¹H磁共振波谱(MRS)测量组织乳酸含量时,常因与1.3 ppm处强烈的脂质信号重叠而受到干扰。使用点分辨表面线圈(PRESS)进行单体素定位时,4.1 ppm(-CH)共振峰和1.3 ppm -CH₃共振峰在体素间存在较大的化学位移,导致体素内信号相位相反,进而出现部分信号抵消的情况。为了将化学位移减小到可忽略不计的程度,利用FOCI脉冲编写了一种改进的半激光序列(“FOCI-LASER”,简称为fLASER),即使在临床MRI扫描仪有限的射频幅度特性下,也能实现高射频带宽。进一步改进的MQF-fLASER包括一个选择性多量子滤波器,用于检测乳酸并抑制脂质信号。这些序列在飞利浦3T Achieva TX系统上实现。在脑代谢物溶液中,fLASER乳酸信号是PRESS的2.7倍。MQF-fLASER乳酸信号是fLASER的47%(理论最大值为50%),但仍大于PRESS乳酸信号。在油中,主要的1.3 ppm脂质峰被抑制到小于1%。使用更长的梯度持续时间可增强抑制效果。最小可检测乳酸浓度约为0.5 mM。相干选择梯度需处于魔角,以避免分子间多量子相干产生的大量水信号。在初步的患者测量中,脑肿瘤中常观察到乳酸峰,而宫颈肿瘤中未观察到;脂质信号得到有效抑制。总之,与PRESS相比,fLASER序列在直接检测乳酸方面具有大大优越的灵敏度(对其他代谢物的灵敏度相当),而单体素单次激发的MQF-fLASER序列在检测乳酸方面超越了PRESS,同时消除了大量脂质信号。该序列将增加体内乳酸测量作为靶向抗癌治疗以及组织缺氧测量中的生物标志物的潜力。

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