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口服全氯乙烯后大鼠的定时控制操作性行为:时间进程及其与血液和脑溶剂水平的关系。

Schedule-controlled operant behavior of rats following oral administration of perchloroethylene: time course and relationship to blood and brain solvent levels.

作者信息

Warren D A, Reigle T G, Muralidhara S, Dallas C E

机构信息

Department of Pharmacology and Toxicology, College of Pharmacy, University of Georgia, Athens, 30602-2356, USA.

出版信息

J Toxicol Environ Health. 1996 Mar;47(4):345-62. doi: 10.1080/009841096161690.

Abstract

Previous studies have indicated that human exposure to perchloroethylene (PCE) produces subtle behavioral changes and other neurological effects at concentration at or below the current occupational exposure limit. Since comparable effects in animals may be reflected by changes in schedule-controlled operant behavior, the ability of orally administered PCE to alter fixed-ratio (FR) responding for a food reward was investigated in male Sprague-Dawley rats. Furthermore, since behavioral effects of solvents are likely to be more closely related to blood or target tissue (i.e, brain) concentrations than administered dose, the relationship between the pharmacokinetic distribution of PCE and its effects on operant responding was also evaluated. Rats trained to lever-press for evaporated milk on an FR-40 reinforcement schedule were gavaged with 160 or 480 mg/kg PCE and immediately placed in an operant test cage for 90 min. Separate animals gavaged with equivalent doses of PCE were used to determine profiles of blood and brain concentrations versus time. Perchloroethylene produced changes in responding that varied not only with dose but also among animals receiving the same dose. Changes in the response rates of rats receiving 160 mg/kg PCE were either not readily apparent, restricted to the first 5 min of the operant session, or attributable to gavage stress and the dosing vehicle. However, 480 mg/kg produced either an immediate suppression of responding for 15-30 min before a rapid recovery to control rates or a complete elimination of lever-pressing for the majority of the operant session. Although the two doses of PCE produced markedly different effects on operant behavior during the first 30 min of exposure, differences in brain concentrations of PCE were minimal. Furthermore, the majority of animals receiving 480 mg/kg PCE fully recovered from response suppression while blood and brain levels of the solvent continued to rise. Thus, relationships between blood and brain PCE levels and performance impairment were not discernible over the monitored time course. Since the rapid onset of response suppression suggests that the precipitating event occurs within the first few minutes of exposure, it is possible that altered responding is related to the rate of increase in blood or brain concentrations rather than the absolute solvent concentrations themselves. The relationship between the pharmacokinetic distribution of solvents and their effects on the central nervous system is obviously complex and may involve acute neuronal adaptation as well as the dynamics of solvent distribution among the various body compartments.

摘要

先前的研究表明,人类接触全氯乙烯(PCE)后,在浓度达到或低于当前职业接触限值时,会产生细微的行为变化和其他神经学影响。由于动物身上的类似影响可能会通过受日程控制的操作性行为的变化反映出来,因此研究了经口给予PCE对雄性斯普拉格-道利大鼠为获取食物奖励而进行的固定比率(FR)反应的影响。此外,由于溶剂的行为影响可能与血液或靶组织(即大脑)浓度的关系比与给药剂量的关系更为密切,因此还评估了PCE的药代动力学分布与其对操作性反应的影响之间的关系。将经过训练在FR-40强化日程下按压杠杆以获取蒸发乳的大鼠用160或480mg/kg的PCE灌胃,并立即放入操作性测试笼中90分钟。用给予等量PCE的单独动物来确定血液和大脑浓度随时间的变化情况。全氯乙烯产生的反应变化不仅随剂量不同而不同,而且在接受相同剂量的动物之间也有所不同。接受160mg/kg PCE的大鼠的反应率变化要么不明显,局限于操作性实验的前5分钟,要么归因于灌胃应激和给药载体。然而,480mg/kg要么在快速恢复到对照率之前立即抑制反应15 - 30分钟,要么在大部分操作性实验期间完全消除杠杆按压。尽管在接触的前30分钟内,两种剂量的PCE对操作性行为产生了明显不同的影响,但PCE在大脑中的浓度差异很小。此外,大多数接受480mg/kg PCE的动物从反应抑制中完全恢复,而溶剂的血液和大脑水平继续上升。因此,在所监测的时间过程中,血液和大脑中PCE水平与行为损害之间的关系并不明显。由于反应抑制的快速发作表明引发事件发生在接触的最初几分钟内,所以有可能改变的反应与血液或大脑浓度的增加速率有关,而不是与溶剂的绝对浓度本身有关。溶剂的药代动力学分布与其对中枢神经系统的影响之间的关系显然很复杂,可能涉及急性神经元适应以及溶剂在身体各个腔室之间的分布动态。

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