Nonparametric D-R1-R2 distribution MRI of the living human brain.

Diffusion-relaxation correlation NMR can simultaneously characterize both the microstructure and the local chemical composition of complex samples that contain multiple populations of water. Recent developments on tensor-valued diffusion encoding and Monte Carlo inversion algorithms have made it possible to transfer diffusion-relaxation correlation NMR from small-bore scanners to clinical MRI systems. Initial studies on clinical MRI systems employed 5D D-R1 and D-R2 correlation to characterize healthy brain in vivo. However, these methods are subject to an inherent bias that originates from not including R2 or R1 in the analysis, respectively. This drawback can be remedied by extending the concept to 6D D-R1-R2 correlation. In this work, we present a sparse acquisition protocol that records all data necessary for in vivo 6D D-R1-R2 correlation MRI across 633 individual measurements within 25 min-a time frame comparable to previous lower-dimensional acquisition protocols. The data were processed with a Monte Carlo inversion algorithm to obtain nonparametric 6D D-R1-R2 distributions. We validated the reproducibility of the method in repeated measurements of healthy volunteers. For a post-therapy glioblastoma case featuring cysts, edema, and partially necrotic remains of tumor, we present representative single-voxel 6D distributions, parameter maps, and artificial contrasts over a wide range of diffusion-, R1-, and R2-weightings based on the rich information contained in the D-R1-R2 distributions.

Computing and visualising intra-voxel orientation-specific relaxation-diffusion features in the human brain.

Diffusion MRI techniques are used widely to study the characteristics of the human brain connectome in vivo. However, to resolve and characterise white matter (WM) fibres in heterogeneous MRI voxels remains a challenging problem typically approached with signal models that rely on prior information and constraints. We have recently introduced a 5D relaxation-diffusion correlation framework wherein multidimensional diffusion encoding strategies are used to acquire data at multiple echo-times to increase the amount of information encoded into the signal and ease the constraints needed for signal inversion. Nonparametric Monte Carlo inversion of the resulting datasets yields 5D relaxation-diffusion distributions where contributions from different sub-voxel tissue environments are separated with minimal assumptions on their microscopic properties. Here, we build on the 5D correlation approach to derive fibre-specific metrics that can be mapped throughout the imaged brain volume. Distribution components ascribed to fibrous tissues are resolved, and subsequently mapped to a dense mesh of overlapping orientation bins to define a smooth orientation distribution function (ODF). Moreover, relaxation and diffusion measures are correlated to each independent ODF coordinate, thereby allowing the estimation of orientation-specific relaxation rates and diffusivities. The proposed method is tested on a healthy volunteer, where the estimated ODFs were observed to capture major WM tracts, resolve fibre crossings, and, more importantly, inform on the relaxation and diffusion features along with distinct fibre bundles. If combined with fibre-tracking algorithms, the methodology presented in this work has potential for increasing the depth of characterisation of microstructural properties along individual WM pathways.

Accuracy and precision of statistical descriptors obtained from multidimensional diffusion signal inversion algorithms.

In biological tissues, typical MRI voxels comprise multiple microscopic environments, the local organization of which can be captured by microscopic diffusion tensors. The measured diffusion MRI signal can, therefore, be written as the multidimensional Laplace transform of an intravoxel diffusion tensor distribution (DTD). Tensor-valued diffusion encoding schemes have been designed to probe specific features of the DTD, and several algorithms have been introduced to invert such data and estimate statistical descriptors of the DTD, such as the mean diffusivity, the variance of isotropic diffusivities, and the mean squared diffusion anisotropy. However, the accuracy and precision of these estimations have not been assessed systematically and compared across methods. In this article, we perform and compare such estimations in silico for a one-dimensional Gamma fit, a generalized two-term cumulant approach, and two-dimensional and four-dimensional Monte-Carlo-based inversion techniques, using a clinically feasible tensor-valued acquisition scheme. In particular, we compare their performance at different signal-to-noise ratios (SNRs) for voxel contents varying in terms of the aforementioned statistical descriptors, orientational order, and fractions of isotropic and anisotropic components. We find that all inversion techniques share similar precision (except for a lower precision of the two-dimensional Monte Carlo inversion) but differ in terms of accuracy. While the Gamma fit exhibits infinite-SNR biases when the signal deviates strongly from monoexponentiality and is unaffected by orientational order, the generalized cumulant approach shows infinite-SNR biases when this deviation originates from the variance in isotropic diffusivities or from the low orientational order of anisotropic diffusion components. The two-dimensional Monte Carlo inversion shows remarkable accuracy in all systems studied, given that the acquisition scheme possesses enough directions to yield a rotationally invariant powder average. The four-dimensional Monte Carlo inversion presents no infinite-SNR bias, but suffers significantly from noise in the data, while preserving good contrast in most systems investigated.