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首页> 外文期刊>The Journal of Physiology >Characteristics of thermoregulatory and febrile responses in mice deficient in prostaglandin EP1 and EP3 receptors.
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Characteristics of thermoregulatory and febrile responses in mice deficient in prostaglandin EP1 and EP3 receptors.

机译:缺乏前列腺素EP1和EP3受体的小鼠的体温调节和发热反应的特征。

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Previous studies have disagreed about whether prostaglandin EP1 or EP3 receptors are critical for producing febrile responses. We therefore injected lipopolysaccharide (LPS) at a variety doses (1 microg kg(-1)-1 mg kg(-1)) intraperitoneally (i.p.) into wild-type (WT) mice and mice lacking the EP1 or the EP3 receptors and measured changes in core temperature (Tc) by using telemetry. In WT mice, i.p. injection of LPS at 10 microg kg(-1) increased Tc about 1 degrees C, peaking 2 h after injection. At 100 microg kg(-1), LPS increased Tc, peaking 5-8 h after injection. LPS at 1 mg kg(-1) decreased Tc, reaching a nadir at 5-8 h after injection. In EP1 receptor knockout (KO) mice injected with 10 microg kg(-1) LPS, only the initial (< 40 min) increase in Tc was lacking; with 100 microg kg(-1) LPS the mice showed no febrile response. In EP3 receptor KO mice, LPS decreased Tc in a dose- and time-dependent manner. Furthermore, in EP3 receptor KO mice subcutaneous injection of turpentine did not induce fever. Both EP1 and EP3 receptor KO mice showed a normal circadian cycle of Tc and brief hyperthermia following psychological stress (cage-exchange stress and buddy-removal stress). The present study suggests that both the EP1 and the EP3 receptors play a role in fever induced by systemic inflammation but neither EP receptor is involved in the circadian rise in Tc or psychological stress-induced hyperthermia in mice.
机译:先前的研究对前列腺素EP1或EP3受体对于产生发热反应是否至关重要至关重要。因此,我们腹膜内(ip)以不同剂量(1 microg kg(-1)-1 mg kg(-1))将脂多糖(LPS)注入野生型(WT)小鼠和缺乏EP1或EP3受体和使用遥测技术测量核心温度(Tc)的变化。在野生型小鼠中以10 microg kg(-1)注射LPS会使Tc升高约1摄氏度,注射后2小时达到峰值。在100微克kg(-1)下,LPS的Tc升高,注射后5-8小时达到峰值。 1 mg kg(-1)的LPS降低了Tc,注射后5-8 h达到最低点。在注射了10 microg kg(-1)LPS的EP1受体基因敲除(KO)小鼠中,只有最初的(<40分钟)Tc缺乏。与100微克kg(-1)LPS,小鼠显示没有发热反应。在EP3受体KO小鼠中,LPS以剂量和时间依赖性方式降低Tc。此外,在EP3受体KO小鼠中,皮下注射松节油不会诱发发烧。 EP1和EP3受体KO小鼠均表现出正常的Tc昼夜节律周期和心理应激(笼交换应激和伙伴去除应激)后短暂的体温过高。本研究表明,EP1和EP3受体均在全身性炎症引起的发热中起作用,但EP受体均不参与小鼠Tc的昼夜节律升高或心理应激引起的体温过高。

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