Whole-brain T 2 mapping with radial sampling and retrospective motion correction at 3T

Whole-brain T 2 mapping with radial sampling and retrospective motion correction at 3T

Several barriers prevent the use of whole-brain T mapping in routine use despite increasing interest in this parameter. One of the main barriers is the long scan time resulting in patient discomfort and motion corrupted data. To address this challenge, a method for accurate whole-brain T mapping wit...

Full description

Saved in:
Bibliographic Details
Published in:Magnetic resonance in medicine
Main Authors: Corbin, Nadège, Trotier, Aurelien J, Anandra, Serge, Kadalie, Emile, Dallet, Laurence, Miraux, Sylvain, Ribot, Emeline J
Format: Journal Article
Language:English
Published: United States Wiley 04-10-2024
Subjects:
Bioengineering
Imaging
Life Sciences
Neurons and Cognition
T2 mapping
radial sampling
motion correction
Motion correction
Radial sampling
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:Several barriers prevent the use of whole-brain T mapping in routine use despite increasing interest in this parameter. One of the main barriers is the long scan time resulting in patient discomfort and motion corrupted data. To address this challenge, a method for accurate whole-brain T mapping with a limited acquisition time and motion correction capabilities is investigated. A 3D radial multi-echo spin-echo sequence was implemented with optimized sampling trajectory enabling the estimation of intra-scan motion, subsequently used to correct the raw data. Motion corrected echo images are then reconstructed with linear subspace constrained reconstruction. Experiments were carried out on phantom and volunteers at 3T to evaluate the accuracy of the T estimation, the sensitivity to lesions and the efficiency of the correction on motion corrupted data. Whole-brain T mapping acquired in less than 7 min enabled the depiction of lesions in the white matter with longer T . Data retrospectively corrupted with typical motion traces of pediatric patients highly benefited from the motion correction by reducing the error in T estimates within the lesions. All datasets acquired on seven volunteers, with deliberate motion, also showed that motion corrupted T maps could be improved with the retrospective motion correction both at the voxel level and the structure level. A whole-brain T mapping sequence with retrospective intra-scan motion correction and reasonable acquisition time is proposed. The method necessitates advanced iterative reconstruction strategies but no additional navigator, external device, or increased scan time is required.
ISSN:0740-3194
1522-2594
DOI:10.1002/mrm.30328