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系统 xc- 突变小鼠的行为特征。

Behavioral characterization of system xc- mutant mice.

机构信息

Department of Biological Sciences, University of Illinois at Chicago, SEL 4311 MC 067, 840 West Taylor Street, Chicago, IL 60607, United States.

Department of Biological Sciences, University of Illinois at Chicago, SEL 4311 MC 067, 840 West Taylor Street, Chicago, IL 60607, United States.

出版信息

Behav Brain Res. 2014 May 15;265:1-11. doi: 10.1016/j.bbr.2014.02.010. Epub 2014 Feb 15.

Abstract

The slc7a11 gene encodes xCT, an essential component of 'system xc-', a plasma membrane exchanger that imports cystine and exports glutamate. Slc7a11 is expressed primarily in the brain, but its role there is not clear. We performed behavioral tests on two different strains of homozygous slc7a11 mutant mice ('sut' and 'xCT'), as well as heteroallelic offspring of these two strains ('xCT/sut') and their associated genetic backgrounds. Homozygous sut mutant males showed reduced spontaneous alternation in spontaneous alternation tasks as well as reduced movement in an open field maze, but xCT and xCT/sut strains did not show significant changes in these tasks compared to appropriate controls. Neither xCT nor sut mutants showed differences from controls in rotarod tests. Female behavioral phenotypes were independent of estrus cycle stage. To ensure that homozygous xCT, sut, and xCT/sut strains all represent protein null alleles, we measured whole brain xCT protein levels using immunoblots. xCT, sut and xCT/sut strains showed no detectable xCT protein expression, confirming them as null alleles. Previously published microdialysis experiments showed reduced striatal glutamate in xCT mutants. Using the same methods, we measured reduced interstitial glutamate levels in the striatum but not cerebellum of sut mutants. However, we detected no glutamate change in the striatum or cerebellum of sut/xCT mice. We detected no changes in whole brain EAAT-1, -2, or -3 expression. We conclude that the behavioral and chemical differences exist between slc7a11 mutant strains, but we were unable to definitively attribute any of these differences to loss of system xc-.

摘要

SLC7A11 基因编码 xCT,是“system xc-”的必需组成部分,“system xc-”是一种质膜交换体,可导入胱氨酸并输出谷氨酸。SLC7A11 主要在大脑中表达,但在大脑中的作用尚不清楚。我们对两种不同品系的纯合 slc7a11 突变小鼠(“sut”和“xCT”)以及这两种品系的杂合后代(“xCT/sut”)及其相关遗传背景进行了行为测试。纯合 sut 突变雄性在自发交替任务中显示出自发交替减少,以及在开阔场迷宫中的运动减少,但 xCT 和 xCT/sut 品系与适当的对照相比,在这些任务中没有显示出显著变化。xCT 和 sut 突变体在旋转棒试验中与对照无差异。雌性行为表型与发情周期阶段无关。为了确保纯合 xCT、sut 和 xCT/sut 品系均代表蛋白质无功能等位基因,我们使用免疫印迹法测量全脑 xCT 蛋白水平。xCT、sut 和 xCT/sut 品系均未检测到 xCT 蛋白表达,证实它们为无功能等位基因。先前发表的微透析实验表明 xCT 突变体纹状体谷氨酸减少。使用相同的方法,我们测量到 sut 突变体纹状体但不是小脑的细胞间隙谷氨酸水平降低。然而,我们在 sut/xCT 小鼠的纹状体或小脑未检测到谷氨酸变化。我们未检测到全脑 EAAT-1、-2 或 -3 表达的变化。我们得出结论,slc7a11 突变株之间存在行为和化学差异,但我们无法明确将这些差异归因于 system xc-的缺失。

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