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Feeding exploratory anxiety- and depression-related behaviors are not altered in interleukin-6-deficient male mice

机译:白细胞介素6缺陷型雄性小鼠的进食探索焦虑和抑郁相关行为均未改变

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摘要

Interleukin-6 (IL-6) has been implicated in behavioral responses associated with inflammation, sickness behavior and various nervous system disorders. We studied a range of different behaviors in IL-6-knockout (IL-6ko) and wild-type (WT) male mice. No significant differences were observed in ambulatory, exploratory, and stereotypic activities in home or novel cages, in an open field (OF), in the multicompartment chamber (MCC), or in the elevated plus-maze (EPM). IL-6ko mice shed fewer fecal boli than WT mice in the OF, in novel cages and in the MCC although this effect was not statistically significant in the OF. In novel cages, intraperitoneal (i.p.) injection of IL-6 (1 μg) depressed ambulatory activity slightly more in IL-6ko than in WT mice. Restraint and interleukin-1β (IL-1β, 100 ng i.p.) decreased exploration of mice in the MCC and EPM, but there was no indication of altered sensitivity in IL-6ko mice. No significant differences were detected in the tail suspension and the Porsolt forced swim tests. IL-1β and lipopolysaccharide (LPS 1 μg i.p.) injection depressed sweetened milk and solid food intake similarly in IL-6ko and WT mice, but IL-6 had no effect, suggesting that IL-6 is not involved in these effects of IL-1 or LPS. However, IL-1β and LPS depressed body weight more in WT than in IL-6ko mice. Plasma corticosterone and basal concentrations of catecholamines, indoleamines and their metabolites in several brain regions were similar. The responses in these measures to IL-1β and LPS were also similar, except that there were no significant changes in tryptophan and serotonin metabolism in IL-6ko mice. This may reflect a role for IL-6 in the tryptophan and serotonin responses to IL-1 and LPS. It is concluded that the lack of IL-6 is not associated with substantial alterations in several different mouse behaviors, and in the responses to restraint, IL-1β, IL-6 and LPS.
机译:白介素6(IL-6)与炎症,疾病行为和各种神经系统疾病有关的行为反应有关。我们研究了IL-6基因敲除(IL-6ko)和野生型(WT)雄性小鼠的一系列不同行为。在家庭或新型笼子,开放区域(OF),多隔室(MCC)或高架迷宫(EPM)的活动,探索和定型活动中未观察到显着差异。在OF,新笼子和MCC中,IL-6ko小鼠的粪便比WT小鼠少,尽管在OF中这种作用在统计学上不显着。在新型笼中,IL-6ko腹膜内(i.p.)注射IL-6(1μg)抑制的走动活动比野生型小鼠稍多。约束和白细胞介素1β(IL-1β,100 ng i.p.)减少了MCC和EPM中小鼠的探查,但没有迹象表明IL-6ko小鼠的敏感性有所改变。在尾部悬架和波索尔特强迫游泳测试中未发现明显差异。 IL-1β和脂多糖(LPS 1μgip)注射类似地抑制了IL-6ko和WT小鼠的甜奶和固体食物摄入,但是IL-6没有作用,表明IL-6不参与IL- 1或LPS。然而,与IL-6ko小鼠相比,WT中IL-1β和LPS降低的体重更大。血浆皮质酮和儿茶酚胺,吲哚胺及其代谢产物在几个大脑区域的基本浓度相似。这些措施对IL-1β和LPS的反应也相似,除了IL-6ko小鼠的色氨酸和5-羟色胺代谢没有明显变化。这可能反映了IL-6在色氨酸和血清素对IL-1和LPS的应答中的作用。结论是缺乏IL-6与几种不同的小鼠行为以及对约束,IL-1β,IL-6和LPS的反应的实质性改变无关。

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