| Literature DB >> 31431689 |
Niki Halttunen1, Frederic Lerouge2, Frederic Chaput1, Marc Vandamme3, Szilvia Karpati1, Salim Si-Mohamed4,5, Monica Sigovan4, Loic Boussel4, Emmanuel Chereul3, Philippe Douek4,5, Stephane Parola6.
Abstract
Computed tomography (CT) is a widely used imaging modality. Among the recent technical improvements to increase the range of detection for optimized diagnostic, new devices such as dual energy CT allow elemental discrimination but still remain limited to two energies. Spectral photon-counting CT (SPCCT) is an emerging X-ray imaging technology with a completely new multiple energy detection and high spatial resolution (200 μm). This unique technique allows detection and quantification of a given element thanks to an element-specific increase in X-ray absorption for an energy (K-band) depending on its atomic number. The main contrast media used hitherto are iodine-based compounds but the K-edge of iodine (33.2 keV) is out of the range of detection. Therefore, it is crucial to develop contrast media suitable for this advanced technology. Gadolinium, well known and used element for MRI, possess a K-edge (50.2 keV) well suited for the SPCCT modality. The use of nano-objects instead of molecular entities is pushed by the necessity of high local concentration. In this work, nano-GdF3 is validated on a clinical based prototype, to be used as efficient in vivo contrast media. Beside an extremely high stability, it presents long lasting time in the blood pool allowing perfusion imaging of small animals, without apparent toxicity.Entities:
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Year: 2019 PMID: 31431689 PMCID: PMC6702219 DOI: 10.1038/s41598-019-48641-z
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379
Figure 1Transmission Electron Microscopy of GdF3 nanoparticles (left); High resolution of the crystalline nanoparticles (middle) and powder X-Ray Diffraction pattern (right).
Figure 2Calibration of GdF3, radio opacity measurements (HU) as a function of Gadolinium concentration. The right plot represents a zoom section of the 0–12 mg/mL range issued from the left plot.
Figure 3In vivo monitoring and CT images of the hybrid nano-GdF3 particles in the Heart (top left), the liver (top right), the kidney (bottom). CT images at T = 0 and 1 minute are shown in Fig. 4.
Figure 4CT images at T = 0 and 1 minute.
Figure 5(Left) SPCCT gadolinium K-edge image of a phantom consisting of GdF3 suspensions of various gadolinium concentrations from 2 mg/mL up to 20 mg/mL (12 mM to 120 mM respectively) (Right) Same phantom observed with SPCCT conventional image.
Figure 6Correlation between measured concentration of gadolinium with K-edge and expected concentrations of the corresponding solutions determined by ICP.
Figure 7SPCCT conventional HU image (A) SPCCT gadolinium K-edge image (B) and overlay between SPCCT conventional HU and Gd K-edge images (C) of abdomen of rat after GdF3 injection (5 min). Both images are reconstructed on an isotropic voxel grid at 250 µm * 250 µm * 250 µm.
Figure 8Delimited box (in red) for Gd3+ quantification in the aorta.