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氟烷可降低白蛋白和转铁蛋白的合成:对离体灌注大鼠肝脏和完整大鼠的研究。

Halothane decreases albumin and transferrin synthesis: studies in the isolated, perfused rat liver and in the intact rat.

作者信息

Franks J J, Kruskal J B, Kirsch R E, Beechey A P, Morrell D F, Harrison G G

机构信息

Department of Anesthesiology, Vanderbilt University, Nashville, Tennessee 37232.

出版信息

Anesthesiology. 1988 Apr;68(4):529-33. doi: 10.1097/00000542-198804000-00009.

Abstract

Isolated perfused rat livers exposed to 1.5% halothane (equivalent to 1.35 MAC) in O2/CO2 or to O2/CO2 alone produced urea, as well as albumin and transferrin (both measured by immunodiffusion), at constant rates during a 4.25-h perfusion. Urea production did not differ in the two treatment groups, but halothane depressed albumin and transferrin synthesis 43% and 45%, respectively. Intact rats were also exposed to halothane, after which albumin synthesis was measured by the (14C)carbonate technique. The minimum halothane concentration required to insure sufficient relaxation for ventilation was selected and ranged from 1.0 to 1.5%. Measurements were made in control rats not exposed to halothane (group I) and in halothane exposed rats immediately after 1 h of anesthesia (group II), 24 h after the start of 1 h of anesthesia (group III), and immediately after 1/2 h of anesthesia preceded by a 1-h exposure 24 h earlier (group IV). Single exposures to halothane (groups II and III) resulted in a decrease in albumin synthesis immediately or 24 h later that did not differ significantly from controls (group I). However, halothane given twice to rats at 24-h intervals (group IV) reduced their mean albumin synthesis rate to half that of controls. The early onset and constancy of halothane depression of export protein synthesis by isolated, perfused livers may reflect a response to halothane itself, rather than an effect resulting from the accumulation of halothane metabolites. Similarly, reduction of albumin synthesis in intact rats immediately after a second halothane exposure may indicate a response to halothane, rather than to halothane metabolites.

摘要

在4.25小时的灌注过程中,将离体灌注的大鼠肝脏暴露于含1.5%氟烷(相当于1.35倍最低肺泡有效浓度)的氧气/二氧化碳混合气中,或仅暴露于氧气/二氧化碳混合气中,肝脏会以恒定速率产生尿素、白蛋白和转铁蛋白(两者均通过免疫扩散法测定)。两个处理组的尿素生成没有差异,但氟烷使白蛋白和转铁蛋白的合成分别降低了43%和45%。完整的大鼠也暴露于氟烷中,之后通过(14C)碳酸盐技术测定白蛋白的合成。选择确保通气充分松弛所需的最低氟烷浓度,范围为1.0%至1.5%。在未暴露于氟烷的对照大鼠(I组)以及在麻醉1小时后立即(II组)、麻醉开始1小时后24小时(III组)和在24小时前先暴露1小时后再麻醉半小时后立即(IV组)的氟烷暴露大鼠中进行测量。单次暴露于氟烷(II组和III组)导致白蛋白合成立即或24小时后降低,但与对照组(I组)相比无显著差异。然而,以24小时间隔给大鼠两次氟烷(IV组),其平均白蛋白合成速率降至对照组的一半。离体灌注肝脏中氟烷对输出蛋白合成的早期发作和持续性抑制可能反映了对氟烷本身的反应,而不是氟烷代谢产物积累产生的影响。同样,完整大鼠在第二次氟烷暴露后立即白蛋白合成减少可能表明是对氟烷的反应,而不是对氟烷代谢产物的反应。

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