Effect of metabolic cage housing on immunoglobulin A and corticosterone excretion in faeces and urine of young male rats

Eriksson, Emma; Royo, Félix; Lyberg, K.; Carlsson, Hans‐Erik; Hau, Jann

doi:10.1113/expphysiol.2004.027656

Cited by 81 publications

(61 citation statements)

References 27 publications

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“…The Cryptochrome (Cry) and Clock genes are proposed to be part of the core clock as well as the Per genes (Albrecht 2004), which suggests that the corticosterone rhythm might, to some degree, be dependent on a fully functional clock. It might be argued that the metabolic cage represents a stressor for the mice as it has been shown to be the case for rats (Eriksson et al 2004). In order to avoid such an effect, the habituation period of 4 days was chosen even 1 day longer than previously shown as affective (Touma et al 2004).…”

Section: Glucose Tolerance Testmentioning

confidence: 99%

Impaired daily glucocorticoid rhythm in Per1 Brd mice

et al. 2006

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Biological clocks have evolved in all kinds of organisms in order to anticipate and adjust to the daily light-dark cycle. Within the last decade, the molecular machinery underlying the circadian system was unraveled. In the present study, the impact of the loss of the Per1 or Per2 genes, key components of the core clock oscillator, on body mass, food and water intake, glucose metabolism, and hypothalamic-pituitary-adrenal axis, was investigated in the Per1 Brd and Per2 Brd mouse models. The results reveal that the lack of Per1 but not Per2 has severe consequences for the regulation of these parameters. Specifically, in Per1 Brd animals, we found an impaired daily glucocorticoid rhythm, with markedly elevated levels during the day compared to control animals. In addition, Per1 Brd mice showed significant differences in body mass as well as food and water intake. Although the Per1 Brd are lighter than wildtype mice, food and water intake per gram body mass is elevated. In addition, the Per1 Brd mice exhibit an increased glucose metabolism after i.p. injection with glucose. In conclusion, our study presents first evidence for a link between an altered metabolism in Per1 and Per2 deficient mice, which in the case of the Per1 Brd animals might be due to an impaired corticosterone rhythm.

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Section: Glucose Tolerance Testmentioning

confidence: 99%

Impaired daily glucocorticoid rhythm in Per1 Brd mice

et al. 2006

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“…24,[30][31][32][33][34][35][36][37][38] This modification exerted only a limited impact on the biokinetics of PAA-PEG and PAA NPs since most of these NPs in the brain were in residual blood. However, in contrast, the amounts of gold and TiO 2 NPs in the brain cannot be explained by differences in the content of residual blood, which lends support to a permeability greater than zero.…”

mentioning

confidence: 99%

Toward a general physiologically-based pharmacokinetic model for intravenously injected nanoparticles

Carlander

Jolliet

et al. 2016

IJN

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To assess the potential toxicity of nanoparticles (NPs), information concerning their uptake and disposition (biokinetics) is essential. Experience with industrial chemicals and pharmaceutical drugs reveals that biokinetics can be described and predicted accurately by physiologically-based pharmacokinetic (PBPK) modeling. The nano PBPK models developed to date all concern a single type of NP. Our aim here was to extend a recent model for pegylated polyacrylamide NP in order to develop a more general PBPK model for nondegradable NPs injected intravenously into rats. The same model and physiological parameters were applied to pegylated polyacrylamide, uncoated polyacrylamide, gold, and titanium dioxide NPs, whereas NP-specific parameters were chosen on the basis of the best fit to the experimental time-courses of NP accumulation in various tissues. Our model describes the biokinetic behavior of all four types of NPs adequately, despite extensive differences in this behavior as well as in their physicochemical properties. In addition, this simulation demonstrated that the dose exerts a profound impact on the biokinetics, since saturation of the phagocytic cells at higher doses becomes a major limiting step. The fitted model parameters that were most dependent on NP type included the blood:tissue coefficients of permeability and the rate constant for phagocytic uptake. Since only four types of NPs with several differences in characteristics (dose, size, charge, shape, and surface properties) were used, the relationship between these characteristics and the NPdependent model parameters could not be elucidated and more experimental data are required in this context. In this connection, intravenous biodistribution studies with associated PBPK analyses would provide the most insight.

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“…The amount of radioactivity detected in feces was highest and displayed a more pronounced peak 12h after injection when the substance was administered through a jugular vein catheter than through tail vein injection. As expected, it is evident that there were great differences in the profiles of radioactive excretion among individuals in rodents, particularly in well studied species such rats and mice, as in others mammals (Brown et al, 1994;Palme et al, 1996), i.e., time course may change with the route and time of administration, even between sexes in some species (see detailed studies on rats: Touma et al, 2003;Eriksson et al, 2004;Abelson et al, 2009). Similarly, in chinchilla, Busso et al (2005a also indicated that radioactive urinary estradiol peaked between 24-48h, the radioactive peak being at 34h post-infusion.…”

Section: Sciurognathi (Squirrel and Mouse-like Forms)mentioning

confidence: 93%