首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Behavioral, neuroendocrine and serotonergic consequences of single social defeat and repeated fluoxetine pretreatment in the Lewis rat strain.
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Behavioral, neuroendocrine and serotonergic consequences of single social defeat and repeated fluoxetine pretreatment in the Lewis rat strain.

机译:在Lewis大鼠品系中,一次社交失误和重复氟西汀预处理对行为,神经内分泌和血清素的影响。

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We have analysed some behavioral, neuroendocrine and serotonergic consequences of a single (30-min) social defeat followed by 14-18 h of sensory contact with the aggressor, in Lewis rats, an inbred strain highly sensitive to chronic social stressors [Berton O. et al. (1998) Neuroscience 82, 147-159]. In addition, we have investigated how the aforementioned consequences are affected by pretreatment with the selective serotonin reuptake inhibitor, fluoxetine (7.5 mg/kg/day for 21 days). A single social defeat triggered hypophagia and body weight loss, and increased anxiety in the elevated plus-maze. It did not affect baseline plasma adrenocorticotropic hormone levels and renin activity, but decreased plasma corticosterone levels. On the other hand, the responses of the latter variables to subsequent acute forced swim stress were blunted (corticosterone) or amplified (adrenocorticotropic hormone, renin activity) by prior defeat. The density of hippocampal serotonin transporters, but not that of hippocampal serotonin-1A and cortical serotonin-2A receptors, was decreased by a single social defeat; in addition, neither tryptophan availability and serotonin synthesis/metabolism, nor serotonin-1A autoreceptor-mediated functions (inhibition of serotonin synthesis, hyperphagia) were affected. Fluoxetine pretreatment diminished social defeat-induced hypophagia, body weight loss and anxiety without affecting these variables in control animals. This pretreatment increased plasma corticosterone levels in resting and acutely stressed rats, but abolished social defeat-elicited corticosterone hyporesponsiveness to acute forced swim stress. Except for a decrease in midbrain serotonin transporter density, fluoxetine did not affect the other serotonergic indices analysed herein, i.e. serotonin-1A and serotonin-2A receptor densities, serotonin synthesis/metabolism. A single social defeat in Lewis rats produces behavioral and endocrine alterations that may model some aspects of human anxiety disorders. In this paradigm, prior fluoxetine treatment is endowed with adaptive behavioral, and possibly neuroendocrine, effects without affecting the key elements of central serotonergic systems analysed herein.
机译:我们分析了Lewis大鼠中单次(30分钟)社交失利,然后与侵略者进行14-18 h感官接触的行为,神经内分泌和血清素能的后果,Lewis大鼠是对慢性社会应激源高度敏感的近交系[Berton O.等。 (1998)Neuroscience 82,147-159]。此外,我们研究了选择性5-羟色胺再摄取抑制剂氟西汀(7.5 mg / kg /天,共21天)的预处理如何影响上述后果。一次社交失误引发了吞咽不足和体重减轻,并在高迷迷宫中增加了焦虑感。它不会影响基线血浆促肾上腺皮质激素水平和肾素活性,但会降低血浆皮质酮水平。另一方面,后一种变量对随后的急性强迫游泳压力的反应由于先前的失败而变得钝化(皮质酮)或增强(促肾上腺皮质激素,肾素活性)。一次社交失败导致海马血清素转运蛋白的密度降低,但海马血清素-1A和皮质血清素-2A受体的密度却没有降低。此外,色氨酸的可用性和5-羟色胺的合成/代谢,或5-羟色胺-1A自身受体介导的功能(5-羟色胺合成的抑制,食欲亢进)均不受影响。氟西汀预处理可减少社交失败导致的吞咽不足,体重减轻和焦虑,而不会影响对照动物的这些变量。这种预处理增加了静息和急性应激大鼠的血浆皮质酮水平,但取消了社交失败引起的皮质酮对急性强迫游泳应激反应的低反应性。除中脑5-羟色胺转运蛋白密度降低外,氟西汀不影响本文分析的其他5-羟色胺能指数,即5-羟色胺-1A和5-羟色胺-2A受体密度,5-羟色胺合成/代谢。在Lewis大鼠中,一次社交失利会产生行为和内分泌改变,从而可以模拟人类焦虑症的某些方面。在该范例中,先前的氟西汀治疗具有适应性的行为,并且可能具有神经内分泌作用,而不会影响本文分析的中央血清素能系统的关键要素。

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