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XXY 小鼠的社会行为和性偏好的遗传、激素和代谢组学影响。

Genetic, hormonal, and metabolomic influences on social behavior and sex preference of XXY mice.

机构信息

Department of Medicine, Harbor-UCLA Medical Center and Los Angeles Biomedical Research Institute, Torrance, California, USA.

出版信息

Am J Physiol Endocrinol Metab. 2010 Sep;299(3):E446-55. doi: 10.1152/ajpendo.00085.2010. Epub 2010 Jun 22.

Abstract

XXY men (Klinefelter syndrome) are testosterone deficient, socially isolated, exhibit impaired gender identity, and may experience more homosexual behaviors. Here, we characterize social behaviors in a validated XXY mouse model to understand mechanisms. Sociability and gender preference were assessed by three-chambered choice tasks before and after castration and after testosterone replacement. Metabolomic activities of brain and blood were quantified through fractional synthesis rates of palmitate and ribose (GC-MS). XXY mice exhibit greater sociability than XY littermates, particularly for male mice. The differences in sociability disappear after matching androgen exposure. Intact XXY, compared with XY, mice prefer male mice odors when the alternatives are ovariectomized female mice odors, but they prefer estrous over male mice odors, suggesting that preference for male mice may be due to social, not sexual, cues. Castration followed by testosterone treatment essentially remove these preferences. Fractional synthesis rates of palmitate are higher in the hypothalamus, amygdala, and hippocampus of XXY compared with XY mice but not with ribose in these brain regions or palmitate in blood. Androgen ablation in XY mice increases fractional synthesis rates of fatty acids in the brain to levels indistinguishable from those in XXY mice. We conclude that intact XXY mice exhibit increased sociability, differences in gender preference for mice and their odors are due to social rather than sexual cues and, these differences are mostly related to androgen deficiency rather than genetics. Specific metabolic changes in brain lipids, which are also regulated by androgens, are observed in brain regions that are involved in these behaviors.

摘要

XXY 男性(克莱恩费尔特综合征)睾酮缺乏,社会孤立,表现出性别认同障碍,并且可能表现出更多的同性恋行为。在这里,我们通过验证的 XXY 小鼠模型来描述社会行为,以了解其机制。在去势前后和睾酮替代后,通过三室选择任务评估社交能力和性别偏好。通过棕榈酸和核糖的分数合成率(GC-MS)量化大脑和血液的代谢活性。XXY 小鼠比 XY 同窝仔鼠表现出更强的社交能力,特别是雄性小鼠。在匹配雄激素暴露后,这种社交能力的差异消失了。与 XY 相比,完整的 XXY 小鼠更喜欢雄性小鼠的气味,而当替代物是去势雌性小鼠的气味时,但它们更喜欢发情期的雄性小鼠气味而不是雄性小鼠气味,这表明对雄性小鼠的偏好可能是由于社交而不是性线索。去势后用睾酮治疗基本上消除了这些偏好。与 XY 相比,XXY 小鼠的下丘脑、杏仁核和海马中的棕榈酸分数合成率较高,但这些脑区的核糖或血液中的棕榈酸则不然。雄激素在 XY 小鼠中的消融增加了脂肪酸在大脑中的分数合成率,使其与 XXY 小鼠中的水平无法区分。我们得出结论,完整的 XXY 小鼠表现出增加的社交能力,对小鼠及其气味的性别偏好差异归因于社交而不是性线索,这些差异主要与雄激素缺乏有关,而不是遗传因素。在涉及这些行为的脑区观察到大脑脂质的特定代谢变化,这些变化也受雄激素调节。

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