推进丘脑核分割:压缩感知对MRI处理的影响。

IF 3.5 2区 医学 Q1 NEUROIMAGING Human Brain Mapping Pub Date : 2024-12-25 DOI:10.1002/hbm.70120
Sebastian Hübner, Stefano Tambalo, Lisa Novello, Tom Hilbert, Tobias Kober, Jorge Jovicich
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引用次数: 0

摘要

丘脑是灰质核的集合,在感觉运动加工和皮层活动调节中起着至关重要的作用。结构MRI无创表征丘脑核对帕金森病、癫痫、痴呆和精神分裂症患者尤其重要。然而,这些种群中严重的头部运动对丘脑核的体内定位提出了重大挑战。最近的进展是利用压缩感知(CS)框架来加快MPRAGE序列变体的结构MRI采集时间,而FastSurfer等快速分割工具减少了神经成像研究的处理时间。在这项研究中,我们评估了六种不同的MPRAGE变体在不同程度的CS加速(从大约9到大约1分钟的获取)下产生的丘脑核分割。分别从FastSurfer和FreeSurfer中初始化丘脑核分割,并评估丘脑核分割工具对不同初始化输入的鲁棒性。我们的发现显示了最小的序列效应,没有系统偏差,整个丘脑和主要丘脑核的序列之间的体积变异性很低。值得注意的是,与非cs序列相比,cs加速序列产生的可变体积更小。此外,FastSurfer和FreeSurfer初始化的丘脑核分割具有高度可比性。我们提供了第一个证据,支持在临床3T MRI系统中使用CS t1加权图像加速对丘脑核进行良好的分割质量是可能的。我们的发现鼓励了未来快速t1加权MRI在研究深部灰质方面的应用。cs加速序列和快速分割方法是未来研究的有前途的工具,旨在表征健康个体和临床人群体内3T时的丘脑核。
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Advancing Thalamic Nuclei Segmentation: The Impact of Compressed Sensing on MRI Processing

The thalamus is a collection of gray matter nuclei that play a crucial role in sensorimotor processing and modulation of cortical activity. Characterizing thalamic nuclei non-invasively with structural MRI is particularly relevant for patient populations with Parkinson's disease, epilepsy, dementia, and schizophrenia. However, severe head motion in these populations poses a significant challenge for in vivo mapping of thalamic nuclei. Recent advancements have leveraged the compressed sensing (CS) framework to accelerate structural MRI acquisition times in MPRAGE sequence variants, while fast segmentation tools like FastSurfer have reduced processing times in neuroimaging research. In this study, we evaluated thalamic nuclei segmentations derived from six different MPRAGE variants with varying degrees of CS acceleration (from about 9 to about 1-min acquisitions). Thalamic segmentations were initialized from either FastSurfer or FreeSurfer, and the robustness of the thalamic nuclei segmentation tool to different initialization inputs was evaluated. Our findings show minimal sequence effects with no systematic bias, and low volume variability across sequences for the whole thalamus and major thalamic nuclei. Notably, CS-accelerated sequences produced less variable volumes compared to non-CS sequences. Additionally, segmentations of thalamic nuclei initialized from FastSurfer and FreeSurfer were highly comparable. We provide the first evidence supporting that a good segmentation quality of thalamic nuclei with CS T1-weighted image acceleration in a clinical 3T MRI system is possible. Our findings encourage future applications of fast T1-weighted MRI to study deep gray matter. CS-accelerated sequences and rapid segmentation methods are promising tools for future studies aiming to characterize thalamic nuclei in vivo at 3T in both healthy individuals and clinical populations.

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来源期刊
Human Brain Mapping
Human Brain Mapping 医学-核医学
CiteScore
8.30
自引率
6.20%
发文量
401
审稿时长
3-6 weeks
期刊介绍: Human Brain Mapping publishes peer-reviewed basic, clinical, technical, and theoretical research in the interdisciplinary and rapidly expanding field of human brain mapping. The journal features research derived from non-invasive brain imaging modalities used to explore the spatial and temporal organization of the neural systems supporting human behavior. Imaging modalities of interest include positron emission tomography, event-related potentials, electro-and magnetoencephalography, magnetic resonance imaging, and single-photon emission tomography. Brain mapping research in both normal and clinical populations is encouraged. Article formats include Research Articles, Review Articles, Clinical Case Studies, and Technique, as well as Technological Developments, Theoretical Articles, and Synthetic Reviews. Technical advances, such as novel brain imaging methods, analyses for detecting or localizing neural activity, synergistic uses of multiple imaging modalities, and strategies for the design of behavioral paradigms and neural-systems modeling are of particular interest. The journal endorses the propagation of methodological standards and encourages database development in the field of human brain mapping.
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