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定量大分子和弥散 MRI 评估的正常髓鞘形成和轴突发育的时间轨迹:兔模型的超微结构和免疫化学验证。

Temporal trajectories of normal myelination and axonal development assessed by quantitative macromolecular and diffusion MRI: Ultrastructural and immunochemical validation in a rabbit model.

机构信息

Department of Pediatrics, NorthShore University HealthSystem Research Institute, Evanston, IL, USA.

Department of Pediatrics, NorthShore University HealthSystem Research Institute, Evanston, IL, USA.

出版信息

Neuroimage. 2023 Apr 15;270:119974. doi: 10.1016/j.neuroimage.2023.119974. Epub 2023 Feb 26.

Abstract

INTRODUCTION

Quantitative and non-invasive measures of brain myelination and maturation during development are of great importance to both clinical and translational research communities. While the metrics derived from diffusion tensor imaging, are sensitive to developmental changes and some pathologies, they remain difficult to relate to the actual microstructure of the brain tissue. The advent of advanced model-based microstructural metrics requires histological validation. The purpose of the study was to validate novel, model-based MRI techniques, such as macromolecular proton fraction mapping (MPF) and neurite orientation and dispersion indexing (NODDI), against histologically derived indexes of myelination and microstructural maturation at various stages of development.

METHODS

New Zealand White rabbit kits underwent serial in-vivo MRI examination at postnatal days 1, 5, 11, 18, and 25, and as adults. Multi-shell, diffusion-weighted experiments were processed to fit NODDI model to obtain estimates, intracellular volume fraction (ICVF) and orientation dispersion index (ODI). Macromolecular proton fraction (MPF) maps were obtained from three source (MT-, PD-, and T1-weighted) images. After MRI sessions, a subset of animals was euthanized and regional samples of gray and white matter were taken for western blot analysis, to determine myelin basic protein (MBP), and electron microscopy, to estimate axonal, myelin fractions and g-ratio.

RESULTS

MPF of white matter regions showed a period of fast growth between P5 and P11 in the internal capsule, with a later onset in the corpus callosum. This MPF trajectory was in agreement with levels of myelination in the corresponding brain region, as assessed by western blot and electron microscopy. In the cortex, the greatest increase of MPF occurred between P18 and P26. In contrast, myelin, according to MBP western blot, saw the largest hike between P5 and P11 in the sensorimotor cortex and between P11 and P18 in the frontal cortex, which then seemingly plateaued after P11 and P18 respectively. G-ratio by MRI markers decreased with age in the white matter. However, electron microscopy suggest a relatively stable g-ratio throughout development.

CONCLUSION

Developmental trajectories of MPF accurately reflected regional differences of myelination rate in different cortical regions and white matter tracts. MRI-derived estimation of g-ratio was inaccurate during early development, likely due to the overestimation of axonal volume fraction by NODDI due to the presence of a large proportion of unmyelinated axons.

摘要

简介

定量和非侵入性的脑髓鞘形成和成熟度测量在临床和转化研究领域都非常重要。虽然来自弥散张量成像的指标对发育变化和一些病理学敏感,但它们仍然难以与脑组织的实际微观结构相关联。先进的基于模型的微观结构指标的出现需要组织学验证。本研究的目的是验证新型的基于模型的 MRI 技术,如大分子质子分数映射(MPF)和神经丝取向和分散指数(NODDI),与不同发育阶段的组织学衍生的髓鞘形成和微观结构成熟度指标相吻合。

方法

新西兰白兔幼仔在出生后第 1、5、11、18 和 25 天以及成年后进行了一系列的活体 MRI 检查。多壳层、弥散加权实验被处理以拟合 NODDI 模型,以获得估计值、细胞内体积分数(ICVF)和取向弥散指数(ODI)。大分子质子分数(MPF)图谱从三个源(MT-、PD-和 T1 加权)图像中获得。在 MRI 检查后,一小部分动物被安乐死,取灰白质的区域样本进行免疫印迹分析,以确定髓鞘碱性蛋白(MBP),和电子显微镜检查,以评估轴突、髓鞘分数和 g-比值。

结果

白质区域的 MPF 在壳核内显示出 P5 至 P11 之间的快速增长期,而胼胝体的增长期较晚。这个 MPF 轨迹与相应脑区的髓鞘化水平相吻合,这是通过免疫印迹和电子显微镜评估的。在皮质中,MPF 的最大增长发生在 P18 至 P26 之间。相比之下,根据 MBP 免疫印迹,感觉运动皮质中的髓鞘在 P5 至 P11 之间以及额叶皮质中的髓鞘在 P11 至 P18 之间经历了最大的增加,之后在 P11 和 P18 之后分别趋于稳定。MRI 标志物的 g-比值随年龄在白质中下降。然而,电子显微镜显示,g-比值在整个发育过程中相对稳定。

结论

MPF 的发育轨迹准确反映了不同皮质区域和白质束的髓鞘形成率的区域差异。在早期发育过程中,MRI 衍生的 g-比值估计不准确,这可能是由于 NODDI 对轴突体积分数的高估,因为存在大量未髓鞘化的轴突。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6add/10103444/137624a0a472/nihms-1883364-f0001.jpg

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