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Magnetization transfer imaging using non‐balanced SSFP at ultra‐low field
Author(s) -
Balaji Sharada,
Wiley Neale,
Dvorak Adam,
Padormo Francesco,
Teixiera Rui P. A. G.,
Poorman Megan E.,
MacKay Alex,
Wood Tobias,
Cassidy Adam R.,
Traboulsee Anthony,
Li David K. B.,
Vavasour Irene,
Williams Steven C. R.,
Deoni Sean C. L.,
Ljungberg Emil,
Kolind Shan H.
Publication year - 2025
Publication title -
magnetic resonance in medicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.696
H-Index - 225
eISSN - 1522-2594
pISSN - 0740-3194
DOI - 10.1002/mrm.30494
Subject(s) - reproducibility , magnetization transfer , white matter , imaging phantom , magnetic resonance imaging , nuclear medicine , multiple sclerosis , medicine , coefficient of variation , biomarker , nuclear magnetic resonance , intraclass correlation , biomedical engineering , physics , chemistry , radiology , biochemistry , chromatography , psychiatry
Abstract Purpose Ultra‐low field MRI scanners have the potential to improve health care delivery, both through improved access in areas where there are few MRI scanners and allowing more frequent monitoring of disease progression and treatment response. This may be particularly true in white matter disorders, including leukodystrophies and multiple sclerosis, in which frequent myelin‐sensitive imaging, such as magnetization transfer (MT) imaging, might improve clinical care and patient outcomes. Methods We implemented an on‐resonance approach to MT imaging on a commercial point‐of‐care 64 mT scanner using a non‐balanced steady‐state free precession sequence. Phantom and in vivo experiments were used to evaluate and optimize the sequence sensitivity and reproducibility, and to demonstrate in vivo performance and inter‐site reproducibility. Results From phantom experiments, T 1 and T 2 effects were determined to have a negligible effect on the differential MT weighting. MT ratio (MTR) values in white matter were 23.1 ± 1.0% from 10 healthy volunteers, with an average reproducibility coefficient of variation of 1.04%. Normal‐appearing white matter MTR values in a multiple sclerosis participant (21.5 ± 6.2%) were lower, but with a similar spread of values, compared to an age‐matched healthy volunteer (23.3 ± 6.2%). Conclusion An on‐resonance MT imaging approach was developed at 64 mT that can be performed in as little as 4 min. A semi‐quantitative myelin‐sensitive imaging biomarker at this field strength is available for assessing both myelination and demyelination.
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