| Literature DB >> 35884917 |
Roxan F C P A Helderman1,2,3, Mauricio Tobón Restrepo4, Hans M Rodermond1,2,3, Gregor G W van Bochove1,2,3, Daan R Löke1,3, Nicolaas A P Franken1,2,3, H Petra Kok1,3, Pieter J Tanis5,6, Johannes Crezee1,3, Arlene L Oei1,2,3.
Abstract
BACKGROUND: The peritoneum is a common site for the formation of metastases originating from several gastrointestinal and gynecological malignancies. A representative preclinical model to thoroughly explore the pathophysiological mechanisms and to study new treatment strategies is important. A major challenge for such models is defining and quantifying the (total) tumor burden in the peritoneal cavity prior to treatment, since it is preferable to use non-invasive methods. We evaluated ultrasound as a simple and easy-to-handle imaging method for this purpose.Entities:
Keywords: imaging modality; orthotopic animal model; peritoneal cancer index; peritoneal carcinomatosis
Year: 2022 PMID: 35884917 PMCID: PMC9313051 DOI: 10.3390/biomedicines10071610
Source DB: PubMed Journal: Biomedicines ISSN: 2227-9059
Figure 1Schematic overview of the induction and imaging of peritoneal metastases in rats, with corresponding age. After the appropriate number of colorectal cancer cells were cultured, the cells were injected in the intraperitoneal area of the rats. Using ultrasound, the tumor formation was assessed, and when tumors reached the size of 4–6 mm, the PCI was scored. Immediately after the last ultrasound imaging, the PCI score was defined ex vivo.
Figure 2Stepwise movement of probe positions to perform gastrointestinal ultrasound in rats. Before the ultrasound procedure, the abdominal skin was shaved and cleaned with 70% ethanol. For each organ, the probe position with the system output is presented, moving from liver, right kidney, stomach, colon, and left kidney to urinary bladder. In the system output, the organ of interest is highlighted by white measurement marks and/or arrows.
Figure 3Schematic overview of the peritoneal cancer index (PCI) tool to assess the extent of PM in rats.
Figure 4The tumor growth over time is presented for three regions in rat 4 (A). Tumor lesions are indicated with white arrows, and organs are named. The progression in total PCI, lesion size and lesion quantity over time was scored on ultrasound by observer 1 (B).
Figure 5Abdomens of the six rats with corresponding ex vivo PCI scores (A). The total PCI, lesion size and lesion quantity scores predicted on ultrasound by 2 independent observers, as well as the ex vivo scoring, are shown in these graphs (B). PCI scoring was performed by one of the two observers when tumors reached the size of 4–6 mm, followed by the second ultrasound scoring within 3 days after the animal was sacrificed in order to score the PCI ex vivo.
Numerical details on the PCI scoring.
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| Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | |
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| Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | Obs. 1 | Obs.2 | Ex vivo | |
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Figure 6Tumors on ultrasound compared to the ex vivo tumor load. Tumor lesions are indicated with white arrows, and organs are named.