2,109 research outputs found
PVR: Patch-to-Volume Reconstruction for Large Area Motion Correction of Fetal MRI
In this paper we present a novel method for the correction of motion
artifacts that are present in fetal Magnetic Resonance Imaging (MRI) scans of
the whole uterus. Contrary to current slice-to-volume registration (SVR)
methods, requiring an inflexible anatomical enclosure of a single investigated
organ, the proposed patch-to-volume reconstruction (PVR) approach is able to
reconstruct a large field of view of non-rigidly deforming structures. It
relaxes rigid motion assumptions by introducing a specific amount of redundant
information that is exploited with parallelized patch-wise optimization,
super-resolution, and automatic outlier rejection. We further describe and
provide an efficient parallel implementation of PVR allowing its execution
within reasonable time on commercially available graphics processing units
(GPU), enabling its use in the clinical practice. We evaluate PVR's
computational overhead compared to standard methods and observe improved
reconstruction accuracy in presence of affine motion artifacts of approximately
30% compared to conventional SVR in synthetic experiments. Furthermore, we have
evaluated our method qualitatively and quantitatively on real fetal MRI data
subject to maternal breathing and sudden fetal movements. We evaluate
peak-signal-to-noise ratio (PSNR), structural similarity index (SSIM), and
cross correlation (CC) with respect to the originally acquired data and provide
a method for visual inspection of reconstruction uncertainty. With these
experiments we demonstrate successful application of PVR motion compensation to
the whole uterus, the human fetus, and the human placenta.Comment: 10 pages, 13 figures, submitted to IEEE Transactions on Medical
Imaging. v2: wadded funders acknowledgements to preprin
Deep learning-based parameter mapping for joint relaxation and diffusion tensor MR Fingerprinting
Magnetic Resonance Fingerprinting (MRF) enables the simultaneous
quantification of multiple properties of biological tissues. It relies on a
pseudo-random acquisition and the matching of acquired signal evolutions to a
precomputed dictionary. However, the dictionary is not scalable to
higher-parametric spaces, limiting MRF to the simultaneous mapping of only a
small number of parameters (proton density, T1 and T2 in general). Inspired by
diffusion-weighted SSFP imaging, we present a proof-of-concept of a novel MRF
sequence with embedded diffusion-encoding gradients along all three axes to
efficiently encode orientational diffusion and T1 and T2 relaxation. We take
advantage of a convolutional neural network (CNN) to reconstruct multiple
quantitative maps from this single, highly undersampled acquisition. We bypass
expensive dictionary matching by learning the implicit physical relationships
between the spatiotemporal MRF data and the T1, T2 and diffusion tensor
parameters. The predicted parameter maps and the derived scalar diffusion
metrics agree well with state-of-the-art reference protocols. Orientational
diffusion information is captured as seen from the estimated primary diffusion
directions. In addition to this, the joint acquisition and reconstruction
framework proves capable of preserving tissue abnormalities in multiple
sclerosis lesions
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