4.4 Article

Volumetric imaging of myelin in vivo using 3D inversion recovery-prepared ultrashort echo time cones magnetic resonance imaging

期刊

NMR IN BIOMEDICINE
卷 33, 期 10, 页码 -

出版社

WILEY
DOI: 10.1002/nbm.4326

关键词

adiabatic inversion recovery; Myelin imaging; 3D Cones

资金

  1. GE Healthcare
  2. National Institute of Neurological Disorders and Stroke, National Institutes of Health [1R01 NS092650]
  3. Kirschstein NRSA Institutional Research Training Grant, National Institutes of Health [T32 EB005970]
  4. VA Clinical Science and Rehabilitation Research and Development Services [I01CX001388, I01RX002604]

向作者/读者索取更多资源

Direct myelin imaging is promising for characterization of multiple sclerosis (MS) brains at diagnosis and in response to therapy. In this study, a 3D inversion recovery-prepared ultrashort echo time cones (IR-UTE-Cones) sequence was used for both morphological and quantitative imaging of myelin on a clinical 3 T scanner. Myelin powder phantoms with different myelin concentrations were imaged with the 3D UTE-Cones sequence and it showed a strong correlation between concentrations and UTE-Cones signals, demonstrating the ability of the UTE-Cones sequence to directly image myelin in the brain. Quantitative myelin imaging with multi-echo IR-UTE-Cones sequences show similar T-2* values for a D2O-exchanged myelin phantom (T-2* = 0.33 +/- 0.04 ms), ex vivo brain specimens (T-2* = 0.20 +/- 0.04 ms) and in vivo healthy volunteers (T-2* = 0.254 +/- 0.023 ms), further confirming the feasibility of 3D IR-UTE-Cones sequences for direct myelin imaging in vivo. In ex vivo MS brain study, signal loss is observed in MS lesions, which was confirmed with histology. For the in vivo study, the lesions in MS patients also show myelin signal loss using the proposed direct myelin imaging method, demonstrating the clinical potential for MS diagnosis. Furthermore, the measured IR-UTE-Cones signal intensities show a significant difference between normal-appearing white matter in MS patients and normal white matter in volunteers, which cannot be found in clinical used T-2-FLAIR sequences. Thus, the proposed 3D IR-UTE-Cones sequence showed clinical potential for MS diagnosis with the capability of direct myelin detection of the whole brain.

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