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兔脑室内牛磺酸:正常体温、内毒素发热以及由前列腺素E1和苯丙胺引起的体温过高的影响

Intracerebroventricular taurine in rabbits: effects of normal body temperature, endotoxin fever and hyperthermia produced by PGE1 and amphetamine.

作者信息

Harris W S, Lipton J M

出版信息

J Physiol. 1977 Apr;266(2):397-410. doi: 10.1113/jphysiol.1977.sp011773.

Abstract
  1. Intracerebroventricular (I.C.V.) injections of taurine into rabbits resting at an ambient temperature (Ta) of 10 degrees or 23 degrees C caused hypothermia but at 30 degrees C ambient temperature, rectal temperature was unchanged. 2. An I.C.V. bolus of 0=5 mg taurine immediately followed by a slow infusion of taurine (0-01--0-2 mg/min) into rabbits at 23 degrees C ambient temperature caused sedation and peripheral vasodilation and blocked the febrile response to Salmonella typhosa endotoxin (1 microng/kg i.v.). Sustained fevers, characteristic of fevers caused by central administration of pyrogens, developed after taurine infusions were stopped. Control infusions of taurine at the same rates in the same rabbits when they were afebrile had little effect on rectal temperature. 3. An I.C.V. injection of 0-5 mg taurine reduced the hyperthermia caused by prostaglandin E1 (PGE1; 2 microng) given I.C.V. A dose of 5-0 mg not only blocked PGE1 hyperthermia but also caused marked hypothermia. 4. Bilateral injections of taurine into the preoptic/anterior hypothalamic region, at sites where injections of Salmonella typhosa endotoxin caused long-lasting fevers, had no effect on rectal temperature. Similar injections into the reticular substance of the medulla oblongata, in the region believed to be concerned with a secondary temperature control function, were also without effect on body temperature. 5. Taurine (0-5 and 5-0 mg, I.C.V.) had no consistent effect on hyperthermia induced by amphetamine (2 mg/kg, I.V.) 6. We conclude that the hypothermic effect of taurine is not due to an action on the central neurone pool or pools concerned with the integrative control of thermoregulatory effectors. This amino acid appears to inhibit neuronal activity in efferent pathways which control peripheral vasomotor tone and heat production and to depress the level of arousal. Taurine delays the onset and extends the duration of endotoxin-induced fever, perhaps by two separate action: by inhibiting activity in central thermoregulatory pathways and by promoting accumulation of endogenous pyrogen in the brain.
摘要
  1. 给处于10℃或23℃环境温度(Ta)下静息的家兔脑室内(I.C.V.)注射牛磺酸会导致体温过低,但在30℃环境温度下,直肠温度未发生变化。2. 在23℃环境温度下,给家兔脑室内快速推注0.5mg牛磺酸,随后缓慢输注牛磺酸(0.01 - 0.2mg/分钟),会引起镇静和外周血管舒张,并阻断对伤寒沙门氏菌内毒素(1μg/kg静脉注射)的发热反应。在停止牛磺酸输注后,出现了由中枢给予致热原引起的持续性发热的典型特征。在相同家兔处于无热状态时,以相同速率进行牛磺酸对照输注对直肠温度几乎没有影响。3. 脑室内注射0.5mg牛磺酸可降低脑室内给予前列腺素E1(PGE1;2μg)所引起的体温过高。5.0mg的剂量不仅能阻断PGE1引起的体温过高,还会导致明显的体温过低。4. 在视前区/下丘脑前部区域,即注射伤寒沙门氏菌内毒素会引起持久发热的部位,双侧注射牛磺酸对直肠温度没有影响。在延髓网状结构中,即在被认为与次级体温调节功能有关的区域进行类似注射,对体温也没有影响。5. 脑室内注射牛磺酸(0.5mg和5.0mg)对苯丙胺(2mg/kg静脉注射)引起的体温过高没有一致的影响。6. 我们得出结论,牛磺酸的体温过低效应并非由于对与体温调节效应器的整合控制有关的一个或多个中枢神经元池起作用。这种氨基酸似乎抑制了控制外周血管运动张力和产热的传出途径中的神经元活动,并降低了觉醒水平。牛磺酸可能通过两种不同作用延迟内毒素诱导发热的起始并延长其持续时间:通过抑制中枢体温调节途径中的活动以及通过促进内源性致热原在脑中的积累。

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