神经退行性疾病MRI数据自动分割一例:II型GM1神经节脂质病。

IF 1.6 Q3 CLINICAL NEUROLOGY
NeuroSci Pub Date : 2025-04-03 DOI:10.3390/neurosci6020031
Connor J Lewis, Jean M Johnston, Precilla D'Souza, Josephine Kolstad, Christopher Zoppo, Zeynep Vardar, Anna Luisa Kühn, Ahmet Peker, Zubir S Rentiya, Muhammad H Yousef, William A Gahl, Mohammed Salman Shazeeb, Cynthia J Tifft, Maria T Acosta
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引用次数: 0

摘要

背景:磁共振成像(MRI)数据的体积分析和分割是评估神经系统疾病进展和神经发育的重要工具。全自动分割管道提供更快和更可重复的结果。然而,由于这些分析管道是在由神经典型对照组成的图谱上训练或运行的,因此评估这些方法对神经退行性疾病的准确性是很重要的。在这项研究中,我们比较了五种全自动分割管道,包括FSL, Freesurfer, volBrain, SPM12和SimNIBS,在GM1神经节脂质病患者和神经正常对照组中进行人工分割过程。方法:我们分析了16例幼年GM1神经节脂病患者的45张MRI扫描,8例晚期婴儿GM1神经节脂病患者的11张MRI扫描,以及11例神经正常对照组的19张MRI扫描。我们比较了7个脑结构的结果,包括大脑总量、双侧丘脑、脑室、双侧尾状核、双侧小体核、胼胝体和小脑。结果:我们发现volBrain的vol2Brain管道与全脑、脑室和丘脑的人工分割过程具有最强的相关性。我们还发现Freesurfer的reco -all管道与尾状核的手动分割过程具有最强的相关性。对于小脑,我们发现volBrain的vol2Brain和SimNIBS的headreco的组合具有最强的相关性,这取决于队列。对于透镜状核,我们发现recon-all和FSL的FIRST的组合给出了最强的相关性,这取决于队列。最后,我们发现胼胝体的分割是高度可变的。结论:先前的研究认为自动分割技术是不可靠的,特别是在神经退行性疾病中。然而,在我们的研究中,我们产生的结果与人工分割过程获得的结果相当。虽然由神经放射学家进行的手动分割过程仍然是黄金标准,但我们提出了使用自动化过程的能力和优势的证据,包括分割整个大脑白质或分析大型数据集的能力,这对完全手动处理提出了可行性问题。未来的研究应考虑使用基于人工智能的分割管道来确定其在GM1神经节脂质病、溶酶体贮积症和其他神经退行性疾病中的准确性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Case for Automated Segmentation of MRI Data in Neurodegenerative Diseases: Type II GM1 Gangliosidosis.

Background: Volumetric analysis and segmentation of magnetic resonance imaging (MRI) data is an important tool for evaluating neurological disease progression and neurodevelopment. Fully automated segmentation pipelines offer faster and more reproducible results. However, since these analysis pipelines were trained on or run based on atlases consisting of neurotypical controls, it is important to evaluate how accurate these methods are for neurodegenerative diseases. In this study, we compared five fully automated segmentation pipelines, including FSL, Freesurfer, volBrain, SPM12, and SimNIBS, with a manual segmentation process in GM1 gangliosidosis patients and neurotypical controls.

Methods: We analyzed 45 MRI scans from 16 juvenile GM1 gangliosidosis patients, 11 MRI scans from 8 late-infantile GM1 gangliosidosis patients, and 19 MRI scans from 11 neurotypical controls. We compared the results for seven brain structures, including volumes of the total brain, bilateral thalamus, ventricles, bilateral caudate nucleus, bilateral lentiform nucleus, corpus callosum, and cerebellum.

Results: We found volBrain's vol2Brain pipeline to have the strongest correlations with the manual segmentation process for the whole brain, ventricles, and thalamus. We also found Freesurfer's recon-all pipeline to have the strongest correlations with the manual segmentation process for the caudate nucleus. For the cerebellum, we found a combination of volBrain's vol2Brain and SimNIBS' headreco to have the strongest correlations, depending on the cohort. For the lentiform nucleus, we found a combination of recon-all and FSL's FIRST to give the strongest correlations, depending on the cohort. Lastly, we found segmentation of the corpus callosum to be highly variable.

Conclusions: Previous studies have considered automated segmentation techniques to be unreliable, particularly in neurodegenerative diseases. However, in our study, we produced results comparable to those obtained with a manual segmentation process. While manual segmentation processes conducted by neuroradiologists remain the gold standard, we present evidence to the capabilities and advantages of using an automated process that includes the ability to segment white matter throughout the brain or analyze large datasets, which pose feasibility issues to fully manual processes. Future investigations should consider the use of artificial intelligence-based segmentation pipelines to determine their accuracy in GM1 gangliosidosis, lysosomal storage disorders, and other neurodegenerative diseases.

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