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聚肌苷酸:聚胞苷酸可增强家兔的慢波睡眠。

Polyriboinosinic:polyribocytidylic acid enhances rabbit slow-wave sleep.

作者信息

Krueger J M, Majde J A, Blatteis C M, Endsley J, Ahokas R A, Cady A B

机构信息

Department of Physiology and Biophysics, University of Tennessee, Memphis 38163.

出版信息

Am J Physiol. 1988 Nov;255(5 Pt 2):R748-55. doi: 10.1152/ajpregu.1988.255.5.R748.

Abstract

Drowsiness and fever are common symptoms of many viral diseases. It has been postulated that double-stranded RNA (dsRNA) produced during viral replication may cause these symptoms by direct toxic effects or by inducing interferon (IFN) or other cytokine production. Polyriboinosinic:polyribocytidylic acid (poly I:C), a pyrogenic and IFN-inducing synthetic dsRNA, and polyriboadenylic:polyribouridylic acid (poly A:U), a less effective pyrogen and IFN-inducing substance, were used as models of viral dsRNA to further characterize the physiological response to dsRNA. Poly I:C was injected either intravenously or intracerebroventricularly into rabbits, and electroencephalograph, body movement, and brain temperature were monitored over the next 6 h; blood samples were taken 24 h postinjection. Poly I:C increased slow-wave sleep duration, suppressed rapid-eye-movement sleep, and induced fever but failed to raise plasma Cu. Dose-dependent responses occurred after intravenous or intracerebroventricular injections; minimal effective doses were 0.3 micrograms/kg (iv) and 1.0 ng (icv). Poly A:U failed to alter the sleep or temperature parameters measured. Responses elicited by poly I:C were distinct from those elicited by bacterial products, e.g., endotoxin enhances plasma Cu levels, thus implying different mechanisms. We conclude that poly I:C enhances slow-wave sleep and body temperature without provoking the acute-phase rise in plasma Cu. These effects may be initiated through an IFN-mediated process.

摘要

嗜睡和发热是许多病毒性疾病的常见症状。据推测,病毒复制过程中产生的双链RNA(dsRNA)可能通过直接毒性作用或诱导干扰素(IFN)或其他细胞因子产生而导致这些症状。聚肌苷酸:聚胞苷酸(poly I:C),一种致热且能诱导IFN产生的合成双链RNA,以及聚腺苷酸:聚尿苷酸(poly A:U),一种致热和诱导IFN产生作用较弱的物质,被用作病毒双链RNA的模型,以进一步表征对双链RNA的生理反应。将poly I:C静脉内或脑室内注射到兔子体内,在接下来的6小时内监测脑电图、身体活动和脑温;注射后24小时采集血样。poly I:C增加了慢波睡眠时间,抑制了快速眼动睡眠,并诱导了发热,但未能提高血浆铜水平。静脉内或脑室内注射后出现剂量依赖性反应;最小有效剂量分别为0.3微克/千克(静脉注射)和1.0纳克(脑室内注射)。poly A:U未能改变所测量的睡眠或体温参数。poly I:C引发的反应与细菌产物引发的反应不同,例如内毒素会提高血浆铜水平,这意味着机制不同。我们得出结论,poly I:C可增强慢波睡眠和体温,而不会引发血浆铜的急性期升高。这些作用可能是通过IFN介导的过程启动的。

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