SpinFlowSim: A blood flow simulation framework for histology-informed diffusion MRI microvasculature mapping in cancer

血流 计算机科学 磁共振弥散成像 扩散 医学 人工智能 生物医学工程 磁共振成像 放射科 物理 热力学
作者
Anna Voronova,Athanasios Grigoriou,Kinga Bernatowicz,S. Simonetti,Garazi Serna,Núria Rosón,Manuel Escobar,María Vieito,Paolo Nucíforo,Rodrigo A. Toledo,Elena Garralda,Els Fieremans,Dmitry S. Novikov,Marco Palombo,Raquel Pérez-López,Francesco Grussu
出处
期刊:Medical Image Analysis [Elsevier BV]
卷期号:102: 103531-103531 被引量:1
标识
DOI:10.1016/j.media.2025.103531
摘要

Diffusion Magnetic Resonance Imaging (dMRI) sensitises the MRI signal to spin motion. This includes Brownian diffusion, but also flow across intricate networks of capillaries. This effect, the intra-voxel incoherent motion (IVIM), enables microvasculature characterisation with dMRI, through metrics such as the vascular signal fraction fV or the vascular Apparent Diffusion Coefficient (ADC) D∗. The IVIM metrics, while sensitive to perfusion, are protocol-dependent, and their interpretation can change depending on the flow regime spins experience during the dMRI measurements (e.g., diffusive vs ballistic), which is in general not known for a given voxel. These facts hamper their practical clinical utility, and innovative vascular dMRI models are needed to enable the in vivo calculation of biologically meaningful markers of capillary flow. These could have relevant applications in cancer, as in the assessment of the response to anti-angiogenic therapies targeting tumour vessels. This paper tackles this need by introducing SpinFlowSim, an open-source simulator of dMRI signals arising from blood flow within pipe networks. SpinFlowSim, tailored for the laminar flow patterns within capillaries, enables the synthesis of highly-realistic microvascular dMRI signals, given networks reconstructed from histology. We showcase the simulator by generating synthetic signals for 15 networks, reconstructed from liver biopsies, and containing cancerous and non-cancerous tissue. Signals exhibit complex, non-mono-exponential behaviours, consistent with in vivo signal patterns, and pointing towards the co-existence of different flow regimes within the same network, as well as diffusion time dependence. We also demonstrate the potential utility of SpinFlowSim by devising a strategy for microvascular property mapping informed by the synthetic signals, and focussing on the quantification of blood velocity distribution moments and of an apparent network branching index. These were estimated in silico and in vivo, in healthy volunteers scanned at 1.5T and 3T and in 13 cancer patients, scanned at 1.5T. In conclusion, realistic flow simulations, as those enabled by SpinFlowSim, may play a key role in the development of the next-generation of dMRI methods for microvascular mapping, with immediate applications in oncology.
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