Comparison of small animal CT contrast agents

Comparison of small animal CT contrast agents

Non‐invasive in vivo small animal computed tomography (CT) imaging provides high resolution bone scans but cannot differentiate between soft tissues. For most applications injections of contrast agents (CAs) are necessary. Aim of this study was to uncover the advantages and disadvantages of commerci...

Ausführliche Beschreibung

Gespeichert in:
Bibliographische Detailangaben
Veröffentlicht in:Contrast media and molecular imaging 2016-07, Vol.11 (4), p.272-284
Hauptverfasser: Mannheim, Julia G., Schlichthaerle, Thomas, Kuebler, Laura, Quintanilla‐Martinez, Leticia, Kohlhofer, Ursula, Kneilling, Manfred, Pichler, Bernd J.
Format: Artikel
Sprache:eng
Schlagworte:
Anesthesia
Animals
biodistribution
contrast agents
Contrast Media - adverse effects
Contrast Media - pharmacokinetics
Contrast Media - toxicity
Drug Interactions
Heart Ventricles - diagnostic imaging
Histiocytes - drug effects
Kidney - diagnostic imaging
Liver - diagnostic imaging
Liver - pathology
Mice
Muscles - diagnostic imaging
pharmacokinetics
side‐effects
small animal CT
Spleen - diagnostic imaging
Spleen - pathology
Tomography, X-Ray Computed
X-Ray Microtomography - methods
Online-Zugang:Volltext
Tags: Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
Beschreibung
Zusammenfassung:Non‐invasive in vivo small animal computed tomography (CT) imaging provides high resolution bone scans but cannot differentiate between soft tissues. For most applications injections of contrast agents (CAs) are necessary. Aim of this study was to uncover the advantages and disadvantages of commercially available CT CAs (ExiTron nano 12 000 and 6000, eXIA 160 and 160XL, Fenestra VC and LC) regarding their pharmacokinetics, toxicological side‐effects and the influence of anesthesia on the biodistribution, based on an injection volume of 100 μL/25 g body weight. The pharmacokinetics of the CAs were determined for up to five days. The CA‐induced toxicological/physiological side‐effects were evaluated by determining blood counts, liver enzymes, thyroxine and total protein values, pro‐inflammatory mediators (messenger ribonucleic acid (mRNA)), histology and immunohistochemistry. ExiTron nano 12 000 and 6000 yielded a long‐term contrast enhancement (CE) in the liver and spleen for up to five days. Some of the evaluated CAs did not show any CE at all. Anesthesia did not impair the CAs' biodistribution. The CAs differentially affected the body weight, blood counts, liver enzymes, thyroxine and total protein values. ExiTron nano 12 000 and 6000 induced histiocytes in the liver and spleen. Moreover, ExiTron nano 12 000 and eXIA 160 enhanced tumor necrosis factor (TNF) mRNA expression levels in the kidneys. Thus, we recommend ExiTron nano 12 000 and 6000 when multiple injections should be avoided. We recommend careful selection of the employed CA in order to achieve an acceptable CE in the organs of interest and to avoid influences on the animal physiology. Copyright © 2016 John Wiley & Sons, Ltd. The CT contrast agents ExiTron nano 12 000 and 6000 yielded a long‐term contrast enhancement in the liver and spleen for up to 5 days. Some of the other CAs did not show any CE at all compared to the control group. Shown are representative CT images 120 h after injection of the respective contrast agent.
ISSN:1555-4309
1555-4317
DOI:10.1002/cmmi.1689