To determine the impact of single and cumulative doses of MultiHance on toxicity, pharmacokinetics, tissue gadolinium presence, behavior and neurological function in juvenile rats. Juvenile male and female rats received either physiological saline or MultiHance at 0.6, 1.25 or 2.5 mmol/kg bodyweight. Animals received either single or six consecutive MultiHance administrations and were sacrificed the day after the last administration or after a 60-day treatment-free period. Animals were assessed for behavior, cognitive function, grip strength, gait, pupillary reflex, and auditory reflex, as well as for physical development, sexual maturation and histopathology. Gadolinium presence in brain, femur, kidneys, liver and skin was determined using inductively coupled plasma-mass spectrometry (ICP-MS). No effects of MultiHance on behavior, cognitive function or any other parameter were noted, even for the highest administered cumulative dose (15 mmol/kg). Gadolinium presence was variable across tissues and decreased during the 60-day treatment-free period. The highest levels were noted in the femur and the lowest levels in the brain. Gadolinium presence in juvenile rat brain following single or repeated MultiHance administrations was minimal and non-impactful.
A nephroblastoma is a tumor arising from metanephric blastema occurring in childhood.
Among laboratory rodents, nephroblastoma has been frequently reported in rats, but it
remains exceedingly rare in mice. The present work describes a nephroblastoma in a young
mouse homozygous for the specific Trp53 R172H point mutation coupled with targeted
deletion of the Pin1 gene. The affected kidney was effaced by a biphasic
tumor with an epithelial component arranged in tubules surrounded by nests of blastemal
cells. Immunohistochemically, the neoplasm was diffusely positive for Wilms’ tumor
antigen. The epithelial component expressed markers of renal tubular differentiation
including wide-spectrum cytokeratin, E-cadherin and folate-binding protein. Furthermore,
the neoplasm exhibited a high proliferative index and diffuse nucleocytoplasmic β-catenin
expression. Based on histological and immunohistochemical features, a diagnosis of
nephroblastoma potentially associated with Trp53 loss and oncogenic
β-catenin activation has been proposed.
Background
Gd levels are higher in tissues of animals with compromised renal function, but studies to compare levels after exposure to different macrocyclic gadolinium-based contrast agents (GBCAs) are lacking. We compared Gd levels in tissues of subtotally nephrectomised (SN) rats after repeated exposure to macrocyclic GBCAs.
Methods
Sprague–Dawley SN male rats (19 per group) received 16 injections of gadoteridol, gadobutrol, or gadoterate meglumine at 0.6 mmol Gd/kg 4 times/weeks over 4 weeks. A control group of healthy male rats (n = 10) received gadoteridol at the same dosage. Plasma urea and creatinine levels were monitored. Blood, cerebrum, cerebellum, liver, femur, kidney(s), skin and peripheral nerves were harvested for Gd determination by inductively coupled plasma-mass spectrometry at 28 and 56 days after the end of treatment.
Results
Plasma urea and creatinine levels were roughly twofold higher in SN rats than in healthy rats at all timepoints. At day 28, Gd levels in the peripheral nerves of gadobutrol- or gadoterate-treated SN animals were 5.4 or 7.2 times higher than in gadoteridol-treated animals (p < 0.001). Higher Gd levels after administration of gadobutrol or gadoterate versus gadoteridol were also determined in kidneys (p ≤ 0.002), cerebrum (p ≤ 0.001), cerebellum (p ≤ 0.003), skin (p ≥ 0.244), liver (p ≥ 0.053), and femur (p ≥ 0.271). At day 56, lower Gd levels were determined both in SN and healthy rats for all GBCAs and tissues, except the femur.
Conclusions
Gd tissue levels were lower following gadoteridol exposure than following gadobutrol or gadoterate exposure.
In cooperation with
HistoryA 7-year-old 31-kg (68.2-lb) sexually intact male English Bulldog was referred for evaluation of severe expiratory dyspnea that was unresponsive to treatment with furosemide. The dog had a history of idiopathic juvenile epilepsy and was currently receiving treatment with phenobarbital (100 mg, PO, q 12 h) and bromide (400 mg, PO, q 12 h). At the referral evaluation, the emergency care provided included administration of cephalexin (30 mg/kg [13.6 mg/lb], IV, q 12 h), enrofloxacin (5 mg/kg [2.27 mg/lb], IV, q 12 h), beclomethasone dipropionate (aerosol, q 8 h), butorphanol tartrate (0.2 mg/kg [0.09 mg/lb], IM, single administration), oxygen via nasal probe (65 mL/kg [29.5 mL/lb)]), and fluid therapy (50 mL/kg/24 h [22.7 mL/ lb/24 h)], IV). Despite treatment, the dog developed respiratory arrest 12 hours after admission, and CPR was unsuccessful.
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