Tensor-valued diffusion encoding for diffusional variance decomposition (DIVIDE): Technical feasibility in clinical MRI systems

Filip Szczepankiewicz; Jens Sjölund; Freddy Ståhlberg; Jimmy Lätt; Markus Nilsson

doi:10.1371/journal.pone.0214238

Tensor-valued diffusion encoding for diffusional variance decomposition (DIVIDE): Technical feasibility in clinical MRI systems

PLoS One. 2019 Mar 28;14(3):e0214238. doi: 10.1371/journal.pone.0214238. eCollection 2019.

Authors

Filip Szczepankiewicz¹, Jens Sjölund^{2

3

4}, Freddy Ståhlberg^{1

5}, Jimmy Lätt⁶, Markus Nilsson^{5

7}

Affiliations

¹ Lund University, Department of Clinical Sciences Lund, Medical Radiation Physics, Lund, Sweden.
² Elekta Instrument AB, Kungstensgatan 18, Stockholm, Sweden.
³ Linköping University, Department of Biomedical Engineering, Linköping, Sweden.
⁴ Linköping University, Center for Medical Image Science and Visualization (CMIV), Linköping, Sweden.
⁵ Lund University, Department of Clinical Sciences Lund, Diagnostic Radiology, Lund, Sweden.
⁶ Skåne University Hospital, Department of Imaging and Function, Lund, Sweden.
⁷ Lund University, Lund University Bioimaging Center, Lund, Sweden.

Abstract

Microstructure imaging techniques based on tensor-valued diffusion encoding have gained popularity within the MRI research community. Unlike conventional diffusion encoding-applied along a single direction in each shot-tensor-valued encoding employs diffusion encoding along multiple directions within a single preparation of the signal. The benefit is that such encoding may probe tissue features that are not accessible by conventional encoding. For example, diffusional variance decomposition (DIVIDE) takes advantage of tensor-valued encoding to probe microscopic diffusion anisotropy independent of orientation coherence. The drawback is that tensor-valued encoding generally requires gradient waveforms that are more demanding on hardware; it has therefore been used primarily in MRI systems with relatively high performance. The purpose of this work was to explore tensor-valued diffusion encoding on clinical MRI systems with varying performance to test its technical feasibility within the context of DIVIDE. We performed whole-brain imaging with linear and spherical b-tensor encoding at field strengths between 1.5 and 7 T, and at maximal gradient amplitudes between 45 and 80 mT/m. Asymmetric gradient waveforms were optimized numerically to yield b-values up to 2 ms/μm2. Technical feasibility was assessed in terms of the repeatability, SNR, and quality of DIVIDE parameter maps. Variable system performance resulted in echo times between 83 to 115 ms and total acquisition times of 6 to 9 minutes when using 80 signal samples and resolution 2×2×4 mm3. As expected, the repeatability, signal-to-noise ratio and parameter map quality depended on hardware performance. We conclude that tensor-valued encoding is feasible for a wide range of MRI systems-even at 1.5 T with maximal gradient waveform amplitudes of 33 mT/m-and baseline experimental design and quality parameters for all included configurations. This demonstrates that tissue features, beyond those accessible by conventional diffusion encoding, can be explored on a wide range of MRI systems.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Algorithms*
Brain / diagnostic imaging*
Diffusion Tensor Imaging* / instrumentation
Diffusion Tensor Imaging* / methods
Feasibility Studies
Female
Humans
Image Processing, Computer-Assisted* / instrumentation
Image Processing, Computer-Assisted* / methods
Male
Signal-To-Noise Ratio

Grants and funding

This work was supported by: MN: Swedish Research Council. Grant no. 2016-03443, https://www.vr.se/; MN: Swedish Foundation for Strategic Research. Grant no. AM13-0090, https://strategiska.se/en/; and MN: Random Walk Imaging AB. Grant no MN15, www.rwi.se. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.