We conclude that the three most common T1 mapping protocols produce stable T1 values in phantoms, but not in vivo. To improve the accuracy of T1 mapping, we recommend that sites perform in vivo validation of their T1 mapping method against the inversion recovery reference method, as the first step toward developing a robust calibration scheme.
Research in the macaque monkey suggests that cortical areas with similar microstructure are more likely to be connected. Here, we examine this link in the human cerebral cortex using 2 magnetic resonance imaging (MRI) measures: quantitative T1 maps, which are sensitive to intracortical myelin content and provide an in vivo proxy for cortical microstructure, and resting-state functional connectivity. Using ultrahigh-resolution MRI at 7 T and dedicated image processing tools, we demonstrate a systematic relationship between T1-based intracortical myelin content and functional connectivity. This effect is independent of the proximity of areas. We employ nonlinear dimensionality reduction to characterize connectivity components and identify specific aspects of functional connectivity that are linked to myelin content. Our results reveal a consistent spatial pattern throughout different analytic approaches. While functional connectivity and myelin content are closely linked in unimodal areas, the correspondence is lower in transmodal areas, especially in posteromedial cortex and the angular gyrus. Our findings are in agreement with comprehensive reports linking histologically assessed microstructure and connectivity in different mammalian species and extend them to the human cerebral cortex in vivo.
This work presents a novel approach for modelling laminar myelin patterns in the human cortex in brain MR images on the basis of known cytoarchitecture. For the first time, it is possible to estimate intracortical contrast visible in quantitative ultra-high resolution MR images in specific primary and secondary cytoarchitectonic areas. The presented technique reveals different area-specific signatures which may help to study the spatial distribution of cortical T1 values and the distribution of cortical myelin in general. It may lead to a new discussion on the concordance of cyto- and myeloarchitectonic boundaries, given the absence of such concordance atlases. The modelled myelin patterns are quantitatively compared with data from human ultra-high resolution in-vivo 7T brain MR images (9 subjects). In the validation, the results are compared to one post-mortem brain sample and its ex-vivo MRI and histological data. Details of the analysis pipeline are provided. In the context of the increasing interest in advanced methods in brain segmentation and cortical architectural studies, the presented model helps to bridge the gap between the microanatomy revealed by classical histology and the macroanatomy visible in MRI.
The position of cortical areas can be approximately predicted from cortical surface folding patterns. However, there is extensive inter-subject variability in cortical folding patterns, prohibiting a one-to-one mapping of cortical folds in certain areas. In addition, the relationship between cortical area boundaries and the shape of the cortex is variable, and weaker for higher-order cortical areas. Current surface registration techniques align cortical folding patterns using sulcal landmarks or cortical curvature, for instance. The alignment of cortical areas by these techniques is thus inherently limited by the sole use of geometric similarity metrics. Magnetic resonance imaging T1 maps show intra-cortical contrast that reflects myelin content, and thus can be used to improve the alignment of cortical areas. In this article, we present a new symmetric diffeomorphic multi-contrast multi-scale surface registration (MMSR) technique that works with partially inflated surfaces in the level-set framework. MMSR generates a more precise alignment of cortical surface curvature in comparison to two widely recognized surface registration algorithms. The resulting overlap in gyrus labels is comparable to FreeSurfer. Most importantly, MMSR improves the alignment of cortical areas further by including T1 maps. As a first application, we present a group average T1 map at a uniquely high-resolution and multiple cortical depths, which reflects the myeloarchitecture of the cortex. MMSR can also be applied to other MR contrasts, such as functional and connectivity data.
Highlights
PREVENT-AD is openly releasing datasets to the neuroscience community.
PREVENT-AD is a longitudinal study of older adults at-risk of Alzheimer disease.
Data include imaging, genetics, fluid biochemistry, neurosensory, cognition and more.
Data collection methods and data sharing plans for open science are described.
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.