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小鼠中与社会优势相关的主要尿蛋白及其调控机制。

Social dominance-related major urinary proteins and the regulatory mechanism in mice.

作者信息

Guo Huifen, Fang Qi, Huo Ying, Zhang Yaohua, Zhang Jianxu

机构信息

State Key Laboratory of Integrated Management of Pest Insects and Rodents in Agriculture, Institute of Zoology, Chinese Academy of Sciences, Beijing, China.

出版信息

Integr Zool. 2015 Nov;10(6):543-54. doi: 10.1111/1749-4877.12165.

Abstract

Major urinary proteins (MUPs) have been proven to be non-volatile male pheromones in mice. Here, we aimed to elucidate the relationship between MUPs and dominance hierarchy, and the underlying molecular mechanisms. Dominance-submission relationship was established by chronic dyadic encountering. We found that at the urinary protein level and hepatic mRNA level, the expression of major MUPs, including Mup20, was enhanced in dominant males compared with subordinate males, indicating that MUPs might signal the social status of male mice. Meanwhile, the mRNA level of hepatic corticotropin releasing hormone receptor 2 (CRHR2) was higher in subordinate male mice than in dominant male mice. Castration also enhanced the expression of CRHR2, but suppressed that of MUPs. CRHR2 agonist treatment reduced the expression of MUPs in liver. However, male social status failed to exert significant influence on serum testosterone and corticosterone as well as the mRNA expression of their receptors. These findings reveal that some MUPs, especially Mup20, might constitute potential dominance pheromones and could be downregulated by hepatic CRHR2, which is possibly independent of androgen or corticosterone systems.

摘要

主要尿液蛋白(MUPs)已被证明是小鼠体内的非挥发性雄性信息素。在此,我们旨在阐明MUPs与优势等级之间的关系及其潜在的分子机制。通过长期的二元相遇建立优势-从属关系。我们发现,在尿液蛋白水平和肝脏mRNA水平上,与从属雄性小鼠相比,包括Mup20在内的主要MUPs在优势雄性小鼠中的表达增强,这表明MUPs可能标志着雄性小鼠的社会地位。同时,从属雄性小鼠肝脏中促肾上腺皮质激素释放激素受体2(CRHR2)的mRNA水平高于优势雄性小鼠。去势也增强了CRHR2的表达,但抑制了MUPs的表达。CRHR2激动剂处理降低了肝脏中MUPs的表达。然而,雄性社会地位对血清睾酮和皮质酮及其受体的mRNA表达没有显著影响。这些发现表明,一些MUPs,尤其是Mup20,可能构成潜在的优势信息素,并可能被肝脏CRHR2下调,这可能独立于雄激素或皮质酮系统。

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