Thalamus Optimized Multi Atlas Segmentation (THOMAS): fast, fully automated segmentation of thalamic nuclei from structural MRI

The thalamus and its nuclei are largely indistinguishable on standard T1 or T2 weighted MRI. While diffusion tensor imaging based methods have been proposed to segment the thalamic nuclei based on the angular orientation of the principal diffusion tensor, these are based on echo planar imaging which...

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Bibliographic Details
Published in:NeuroImage (Orlando, Fla.) Fla.), 2019-07, Vol.194, p.272-282
Main Authors: Su, Jason H., Thomas, Francis T., Kasoff, Willard S., Tourdias, Thomas, Choi, Eun Young, Rutt, Brian K., Saranathan, Manojkumar
Format: Article
Language:English
Subjects:
Accuracy
Adult
Alzheimer's disease
Automation
Brain Mapping - methods
Datasets
Female
Humans
Image processing
Image Processing, Computer-Assisted - methods
Localization
Magnetic resonance imaging
Magnetic Resonance Imaging - methods
Male
Methods
Middle Aged
Multi-atlas segmentation
Multiple sclerosis
Neuroimaging
Neurological diseases
Pulvinar
Segmentation
Spatial discrimination
Substantia alba
Surgery
Thalamic nuclei
Thalamic Nuclei - anatomy & histology
Thalamic parcellation
Thalamus
Ultrasonic imaging
Ultrasound
White matter nulled MP-RAGE
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Summary:The thalamus and its nuclei are largely indistinguishable on standard T1 or T2 weighted MRI. While diffusion tensor imaging based methods have been proposed to segment the thalamic nuclei based on the angular orientation of the principal diffusion tensor, these are based on echo planar imaging which is inherently limited in spatial resolution and suffers from distortion. We present a multi-atlas segmentation technique based on white-matter-nulled MP-RAGE imaging that segments the thalamus into 12 nuclei with computation times on the order of 10 min on a desktop PC; we call this method THOMAS (THalamus Optimized Multi Atlas Segmentation). THOMAS was rigorously evaluated on 7T MRI data acquired from healthy volunteers and patients with multiple sclerosis by comparing against manual segmentations delineated by a neuroradiologist, guided by the Morel atlas. Segmentation accuracy was very high, with uniformly high Dice indices: at least 0.85 for large nuclei like the pulvinar and mediodorsal nuclei and at least 0.7 even for small structures such as the habenular, centromedian, and lateral and medial geniculate nuclei. Volume similarity indices ranged from 0.82 for the smaller nuclei to 0.97 for the larger nuclei. Volumetry revealed that the volumes of the right anteroventral, right ventral posterior lateral, and both right and left pulvinar nuclei were significantly lower in MS patients compared to controls, after adjusting for age, sex and intracranial volume. Lastly, we evaluated the potential of this method for targeting the Vim nucleus for deep brain surgery and focused ultrasound thalamotomy by overlaying the Vim nucleus segmented from pre-operative data on post-operative data. The locations of the ablated region and active DBS contact corresponded well with the segmented Vim nucleus. Our fast, direct structural MRI based segmentation method opens the door for MRI guided intra-operative procedures like thalamotomy and asleep DBS electrode placement as well as for accurate quantification of thalamic nuclear volumes to follow progression of neurological disorders. •White-matter nulled MP-RAGE sequence provides improved intra-thalamic contrast.•THOMAS exploits this improved contrast to segment 12 thalamic nuclei with excellent accuracy as measured by Dice against manual segmentation.•Volumetry results using THOMAS revealed atrophy of select nuclei in multiple sclerosis patients.•THOMAS can also be used to accurately predict the ventralis intermedius nucleus f
ISSN:1053-8119
1095-9572
DOI:10.1016/j.neuroimage.2019.03.021