性成熟的完整雄性小鼠的尿液有助于在自由漫游和受限条件下增加心血管反应。

Dexter L Lee, Justin L Wilson
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引用次数: 5

摘要

尿液中的信息素调节雄性老鼠的攻击性,而被阉割的雄性老鼠产生的信息素较少。我们测试了这样一个假设:将性成熟完好(SMI)雄性小鼠的尿液中的信息素放置在单独饲养的雄性小鼠的笼子床上或小鼠约束器中,会导致平均动脉压(MAP)、心率(HR)和活动显著增加。性成熟雄性C57BL/6小鼠植入生物遥测发射器,测量MAP、HR和活性。与去势小鼠诱导的MAP(11±3 mmHg)、HR(70±15 bpm)和activity(5±1计数)相比,将SMI小鼠置于单笼雄性小鼠笼子中的尿液(200 μL)引起MAP(21±4 mmHg)、HR(145±25 bpm)和activity(9 2计数)的基线值显著变化。特拉唑嗪预处理可显著降低重度精神分裂症男性的MAP(9±3 mmHg)、心率(90±15 bpm)和活动(4±2计数)对尿液反应的变化。在任何组中,生理盐水都没有显著增加MAP、HR或活性。在克制期间,重度精神障碍小鼠的尿液引起MAP(5±0.4 mmHg)和HR(17±1 bpm)的显著变化;去势小鼠的尿液没有引起MAP和HR的显著增加。我们的研究结果表明,当雄性小鼠暴露于重度精神分裂症雄性小鼠的尿液信息素时,MAP、HR和活性显著增加。综上所述,在没有与其他雄性小鼠或动物饲养员直接身体接触的情况下,在笼垫和小鼠约束器中排泄的SMI雄性小鼠尿液中的信息素导致心血管反应显著增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Urine from Sexually Mature Intact Male Mice Contributes to Increased Cardiovascular Responses during Free-Roaming and Restrained Conditions.

Urine from Sexually Mature Intact Male Mice Contributes to Increased Cardiovascular Responses during Free-Roaming and Restrained Conditions.

Urine from Sexually Mature Intact Male Mice Contributes to Increased Cardiovascular Responses during Free-Roaming and Restrained Conditions.

Pheromones in the urine regulate aggression of male mice and castrated males produce less of these pheromones. We tested the hypothesis that pheromones in the urine of sexually mature-intact (SMI) males placed in the cage bedding of an individually housed male mouse or in a mouse restrainer would contribute to a significant increase in mean arterial pressure (MAP), heart rate (HR), and activity. Sexually mature male C57BL/6 mice were implanted with a biotelemetry transmitter to measure MAP, HR, and activity. Urine (200 μL) from SMI mice placed in the cages of singularly housed male mice caused significant changes above baseline values for MAP (21 ± 4 mmHg), HR (145 ±25 bpm), and activity (9 2 counts) when compared to urine from castrated mice-induced MAP (11 ± 3 mmHg), HR (70 ± 15 bpm), and activity (5 ± 1 counts). Pretreatment with terazosin significantly reduced the change in MAP (9 ± 3 mmHg), heart rate (90 ± 15 bpm), and activity (4 ± 2 counts) responses to urine from SMI males. Saline did not significantly increase MAP, HR, or activity in any group. During restraint, urine from SMI mice caused a significant change in MAP (5 ±0.4 mmHg) and HR (17 ±1 bpm); urine from castrated mice did not cause a significant increase in MAP and HR. Our results demonstrate that a significant increase in MAP, HR, and activity occurs when male mice are exposed to urine pheromones from SMI males. In summary, pheromones in the urine of SMI male excreted in the cage bedding and mouse restrainers contribute to a significant increase in cardiovascular responses in the absence of direct physical contact with a different male mouse or animal handler.

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