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在针对羊茅中毒具有抗性或易感性而选择的小鼠品系中,麻醉后的睡眠时间。

Sleep time following anesthesia in mouse lines selected for resistance or susceptibility to fescue toxicosis.

作者信息

Arthur K A, Kuehn L A, Hohenboken W D

机构信息

Animal and Poultry Sciences Department, Virginia Polytechnic Institute and State University, Blacksburg 24061-0306, USA.

出版信息

J Anim Sci. 2003 Oct;81(10):2562-7. doi: 10.2527/2003.81102562x.

Abstract

In previous work, a mouse line selected for resistance (R) to fescue toxicosis had higher activities of two hepatic Phase II detoxification enzymes than a mouse line selected for fescue toxicosis susceptibility (S). The primary objective of the present study was to determine whether those same lines also differed in hepatic Phase I enzyme activity, estimated from sleep time (ST) following sodium pentobarbital anesthesia. Additional objectives were to determine whether ST differences between lines were modulated by endophyte-infected fescue in the diet (with or without an enzyme inducer) and whether ST of individual mice was correlated with the effect of a toxin-containing diet on the postweaning growth of those mice. In Exp. I, 24 males from each line were randomly assigned to each of five diets: control (commercial rodent food meal); E+ (50% endophyte-infected fescue seed, 50% control); E+P (the E+ diet supplemented with 1,000 ppm phenobarbital); E- (50% endophyte-free fescue seed, 50% control); and E-P (the E- diet supplemented with 1,000 ppm phenobarbital). After 4 wk on these diets, ST was measured on all the mice. A second ST was recorded on each mouse by randomly sampling one-fourth of the population after 1, 2, 3, or 4 wk on a pelleted rodent food diet. Regardless of diet, R mice had shorter first and second ST than S mice (P < 0.01), suggesting higher hepatic Phase I microsomal enzyme activity. Mice on both phenobarbital-supplemented diets had shorter first ST than mice whose diets did not include that microsomal enzyme inducer (P < 0.01). In Exp. II, ST was measured on male and female R and S mice (n = 280) after they had been fed the E- diet for 2 wk, then the E+ diet for 2 wk, and then a pelleted rodent food diet for 2 wk. Growth response to the E+ diet was the percentage of reduction in gain on the E+ diet compared to gain on the E- diet the previous 2 wk. As in Exp. I, S mice slept longer than R mice (P < 0.01). The residual correlation between ST and gain reduction associated with the E+ diet equaled 0.04. Thus, an animal's apparent Phase I enzyme activity did not predict its growth rate depression on the toxin-containing diet. Based on these and previous studies, divergent selection for toxicosis response in mice was successful partially by causing divergence in activities of hepatic Phase I and II detoxification enzymes.

摘要

在之前的研究中,一个对牛鞭草中毒具有抗性(R)的小鼠品系,其两种肝脏II相解毒酶的活性高于一个对牛鞭草中毒敏感(S)的小鼠品系。本研究的主要目的是确定这两个品系在肝脏I相酶活性方面是否也存在差异,通过戊巴比妥钠麻醉后的睡眠时间(ST)来估算。其他目的是确定品系间的ST差异是否受到饮食中内生菌感染的牛鞭草(有或没有酶诱导剂)的调节,以及个体小鼠的ST是否与含毒素饮食对这些小鼠断奶后生长的影响相关。在实验I中,每个品系的24只雄性小鼠被随机分配到五种饮食中的每一种:对照(商业啮齿动物食物粉);E+(50%内生菌感染的牛鞭草种子,50%对照);E+P(E+饮食添加1000 ppm苯巴比妥);E-(50%无内生菌的牛鞭草种子,50%对照);以及E-P(E-饮食添加1000 ppm苯巴比妥)。在这些饮食上喂养4周后,对所有小鼠测量ST。在以颗粒状啮齿动物食物饮食喂养1、2、3或4周后,通过随机抽取四分之一的群体,对每只小鼠记录第二次ST。无论饮食如何,R小鼠的第一次和第二次ST都比S小鼠短(P < 0.01),表明肝脏I相微粒体酶活性更高。两种添加苯巴比妥的饮食组的小鼠,其第一次ST都比饮食中不包括该微粒体酶诱导剂的小鼠短(P < 0.01)。在实验II中,对雄性和雌性R和S小鼠(n = 280)测量ST,它们先被喂食E-饮食2周,然后喂食E+饮食2周,然后再喂食颗粒状啮齿动物食物饮食2周。对E+饮食的生长反应是E+饮食上的增重相对于前2周E-饮食上的增重减少的百分比。与实验I一样,S小鼠比R小鼠睡眠时间长(P < 0.01)。ST与E+饮食相关的增重减少之间的残差相关性等于0.04。因此,动物的表观I相酶活性并不能预测其在含毒素饮食上的生长速率下降。基于这些以及之前的研究,在小鼠中对中毒反应进行的差异选择部分成功是通过引起肝脏I相和II相解毒酶活性的差异实现的。

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