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1.5T下无病变白质中脑代谢物浓度测量的可重复性

Reproducibility of brain metabolite concentration measurements in lesion free white matter at 1.5 T.

作者信息

Busch Martin H J, Vollmann Wolfgang, Mateiescu Serban, Stolze Manuel, Deli Martin, Garmer Marietta, Grönemeyer Dietrich H W

机构信息

Grönemeyer Institut für Mikrotherapie, Universitätsstraße 142, D-44799, Bochum, Germany.

Beuth Hochschule für Technik Berlin, Luxemburger Straße 10, D-13353, Berlin, Germany.

出版信息

BMC Med Imaging. 2015 Sep 29;15:40. doi: 10.1186/s12880-015-0085-9.

Abstract

BACKGROUND

Post processing for brain spectra has a great influence on the fit quality of individual spectra, as well as on the reproducibility of results from comparable spectra. This investigation used pairs of spectra, identical in system parameters, position and time assumed to differ only in noise. The metabolite amplitudes of fitted time domain spectroscopic data were tested on reproducibility for the main brain metabolites.

METHODS

Proton spectra of white matter brain tissue were acquired with a short spin echo time of 30 ms and a moderate repetition time of 1500 ms at 1.5 T. The pairs were investigated with one time domain post-processing algorithm using different parameters. The number of metabolites, the use of prior knowledge, base line parameters and common or individual damping were varied to evaluate the best reproducibility.

RESULTS

The protocols with most reproducible amplitudes for N-acetylaspartate, creatine, choline, myo-inositol and the combined Glx line of glutamate and glutamine in lesion free white matter have the following common features: common damping of the main metabolites, a baseline using only the points of the first 10 ms, no additional lipid/macromolecule lines and Glx is taken as the sum of separately fitted glutamate and glutamine. This parameter set is different to the one delivering the best individual fit results.

DISCUSSION

All spectra were acquired in "lesion free" (no lesion signs found in MR imaging) white matter. Spectra of brain lesions, for example tumors, can be drastically different. Thus the results are limited to lesion free brain tissue. Nevertheless the application to studies is broad, because small alterations in brain biochemistry of lesion free areas had been detected nearby tumors, in patients with multiple sclerosis, drug abuse or psychiatric disorders.

CONCLUSION

Main metabolite amplitudes inside healthy brain can be quantified with a normalized root mean square deviation around 5 % using CH3 of creatine as reference. Only the reproducibility of myo-inositol is roughly twice as bad. The reproducibility should be similar using other references like internal or external water for an absolute concentration evaluation and are not influenced by relaxation corrections with literature values.

摘要

背景

脑谱的后处理对单个谱的拟合质量以及可比谱结果的可重复性有很大影响。本研究使用了成对的谱,这些谱在系统参数、位置和时间上相同,仅假设噪声不同。对拟合的时域光谱数据的代谢物幅度进行了测试,以检验主要脑代谢物的可重复性。

方法

在1.5T磁场下,采用30ms的短自旋回波时间和1500ms的中等重复时间采集白质脑组织的质子谱。使用一种时域后处理算法,采用不同参数对这些成对谱进行研究。改变代谢物数量、先验知识的使用、基线参数以及共同或个体阻尼,以评估最佳可重复性。

结果

在无病变白质中,对于N-乙酰天门冬氨酸、肌酸、胆碱、肌醇以及谷氨酸和谷氨酰胺的联合Glx线,具有最可重复幅度的方案具有以下共同特征:主要代谢物的共同阻尼、仅使用前10ms点的基线、无额外的脂质/大分子线,并且Glx被视为分别拟合的谷氨酸和谷氨酰胺的总和。此参数集与给出最佳个体拟合结果的参数集不同。

讨论

所有谱均在“无病变”(磁共振成像中未发现病变迹象)的白质中采集。脑病变(例如肿瘤)的谱可能有很大差异。因此,结果仅限于无病变的脑组织。然而,其在研究中的应用广泛,因为在肿瘤附近、患有多发性硬化症、药物滥用或精神疾病的患者中,已检测到无病变区域脑生物化学的微小变化。

结论

以肌酸的CH3为参考,健康脑内主要代谢物幅度可以用约5%的归一化均方根偏差进行量化。只有肌醇的可重复性大约差两倍。使用其他参考物(如内部或外部水)进行绝对浓度评估时,可重复性应相似,且不受文献值的弛豫校正影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/beee/4588462/4ad30b12426a/12880_2015_85_Fig1_HTML.jpg

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