Your search keyword '"Huber, Sabine E"' showing total 2 results

1. The selective FKBP51 inhibitor SAFit2 reduces alcohol consumption and reinstatement of conditioned alcohol effects in mice.

Author

König, Loretta, Kalinichenko, Liubov S., Huber, Sabine E., Voll, Andreas M., Bauder, Michael, Kornhuber, Johannes, Hausch, Felix, and Müller, Christian P.

Subjects

ALCOHOL drinking, ALCOHOLISM, ALCOHOL, GLUCOCORTICOID receptors, MICE, NALTREXONE, ANIMAL behavior, BIOLOGICAL models, RESEARCH, ANIMAL experimentation, RESEARCH methodology, CELL receptors, MEDICAL cooperation, EVALUATION research, SELF medication, COMPARATIVE studies, RESEARCH funding, ETHANOL, CONDITIONED response, CENTRAL nervous system depressants

Abstract

There is still no widely effective pharmacotherapy for alcohol addiction available in the clinic. FK506-binding protein 51 (FKBP51) is a negative regulator of the glucocorticoid receptor signaling pathway that regulates the stress-induced glucocorticoid feedback circuit. Here we asked whether selective inhibitors of FKBP51, exemplified by SAFit2, may serve as a new pharmacological strategy to reduce alcohol consumption and conditioned alcohol effects in a mouse model. We report that a relatively short treatment with SAFit2 (20 mg/kg, ip) reduces ongoing 16 vol% alcohol consumption when administered during free access to alcohol in a two-bottle free-choice test. SAFit2 was also able to reduce alcohol consumption when given during an abstinence period immediately before relapse. In contrast, SAFit2 did not affect alcohol consumption when given during a relapse period after repeated withdrawal from alcohol. SAFit2 (10 and 20 mg/kg, ip) showed no effects when used in an intermittent drinking schedule. When 20 vol% alcohol was only available every other day, SAFit2 had no effect on drinking, no matter whether given during a drinking episode or the day before. SAFit2 (2 and 20 mg/kg, ip) did not affect the expression of an alcohol-induced conditioned place preference (CPP). However, SAFit2 was able to inhibit alcohol-induced reinstatement of an extinguished CPP in a dose-dependent way. Altogether, these data may suggest pharmacological inhibition of FKBP51 as a viable strategy to reduce alcohol seeking and consumption. [ABSTRACT FROM AUTHOR]

Published

2020

2. Prenatal androgen-receptor activity has organizational morphological effects in mice.

Author

Huber, Sabine E., Lenz, Bernd, Kornhuber, Johannes, and Müller, Christian P.

Subjects

*ANDROGEN receptors, *STEROID receptors, *SEX hormones, *FLUTAMIDE, *TESTOSTERONE

Abstract

Prenatal sex hormones exert organizational effects. It has been suggested that prenatal sex hormones affect adult morphological parameters, such as the finger length. Especially the second-to-fourth finger length (2D:4D) ratio has been implicated to be modified when exposed to higher androgen levels in utero. Here we show in a mouse model that experimental manipulation of the prenatal androgen level, by blocking the androgen receptor with flutamide or activating the androgen receptor with dihydrotestosterone (DHT), leads to changes in the length of the fingers of all paws in males and females. In addition to that, also total paw length and the 2D:4D ratio was affected. In males treated with DHT, the 2D:4D ratio was increased, while flutamide-treatment in females led to a reduced 2D:4D ratio. We also measured other parameters, such as head size, body length and tail length and demonstrate that body morphology is affected by prenatal androgen exposure with more prominent effects in females. Another factor that is thought to be influenced by early androgens is handedness. We tested mice for handedness, but did not find a significant effect of the prenatal treatment. These findings demonstrate that prenatal androgen activity is involved in the development of body morphology and might be a useful marker for prenatal androgen exposure. [ABSTRACT FROM AUTHOR]

Published

2017