4.7 Article

Magnetic resonance fingerprinting based on realistic vasculature in mice

期刊

NEUROIMAGE
卷 149, 期 -, 页码 436-445

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.neuroimage.2016.12.060

关键词

Vascular magnetic resonance fingerprinting (vMRF); Superparamagnetic iron oxide nanoparticle (SPION); Gradient-echo sampling of free induction decay and echo (GESFIDE); Mouse model of atherosclerosis; Ab initio Monte Carlo simulations of magnetic resonance signal

资金

  1. NSERC [RGPIN-2014-06089]
  2. CIHR [299166]
  3. NIH [R01-EB021018, R01 NS091230, P01 NS055104]

向作者/读者索取更多资源

Magnetic resonance fingerprinting (MRF) was recently proposed as a novel strategy for MR data acquisition and analysis. A variant of MRF called vascular MRF (vMRF) followed, that extracted maps of three parameters of physiological importance: cerebral oxygen saturation (SatO(2)), mean vessel radius and cerebral blood volume (CBV). However, this estimation was based on idealized 2-dimensional simulations of vascular networks using random cylinders and the empirical Bloch equations convolved with a diffusion kernel. Here we focus on studying the vascular MR fingerprint using real mouse angiograms and physiological values as the substrate for the MR simulations. The MR signal is calculated ab initio with a Monte Carlo approximation, by tracking the accumulated phase from a large number of protons diffusing within the angiogram. We first study the identifiability of parameters in simulations, showing that parameters are fully estimable at realistically high signal-to-noise ratios (SNR) when the same angiogram is used for dictionary generation and parameter estimation, but that large biases in the estimates persist when the angiograms are different. Despite these biases, simulations show that differences in parameters remain estimable. We then applied this methodology to data acquired using the GESFIDE sequence with SPIONs injected into 9 young wild type and 9 old atherosclerotic mice. Both the pre injection signal and the ratio of post-to-pre injection signals were modeled, using 5 dimensional dictionaries. The vMRF methodology extracted significant differences in SatO(2), mean vessel radius and CBV between the two groups, consistent across brain regions and dictionaries. Further validation work is essential before vMRF can gain wider application.

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