首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >A targeted mutation of the D3 dopamine receptor gene is associated with hyperactivity in mice.
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A targeted mutation of the D3 dopamine receptor gene is associated with hyperactivity in mice.

机译:D3多巴胺受体基因的定向突变与小鼠活动过度有关。

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摘要

While most effects of dopamine in the brain are mediated by the D1 and D2 receptor subtypes, other members of this G protein-coupled receptor family have potentially important functions. D3 receptors belong to the D2-like subclass of dopamine receptors, activation of which inhibits adenylyl cyclase. Using targeted mutagenesis in mouse embryonic stem cells, we have generated mice lacking functional D3 receptors. A premature chain-termination mutation was introduced in the D3 receptor gene after residue Arg-148 in the second intracellular loop of the predicted protein sequence. Binding of the dopamine antagonist [125I]iodosulpride to D3 receptors was absent in mice homozygous for the mutation and greatly reduced in heterozygous mice. Behavioral analysis of mutant mice showed that this mutation is associated with hyperactivity in an exploratory test. Homozygous mice lacking D3 receptors display increased locomotor activity and rearing behavior. Mice heterozygous for the D3 receptor mutation show similar, albeit less pronounced, behavioral alterations. Our findings indicate that D3 receptors play an inhibitory role in the control of certain behaviors.
机译:尽管多巴胺在大脑中的大多数作用是由D1和D2受体亚型介导的,但该G蛋白偶联受体家族的其他成员具有潜在的重要功能。 D3受体属于多巴胺受体的D2样亚类,其激活抑制了腺苷酸环化酶。使用小鼠胚胎干细胞中的定向诱变,我们已经生成了缺乏功能性D3受体的小鼠。在预测的蛋白质序列第二个细胞内环的残基Arg-148之后,在D3受体基因中引入了过早的链终止突变。在突变纯合子的小鼠中不存在多巴胺拮抗剂[125I]碘磺化物与D3受体的结合,而在杂合子小鼠中则大大降低。突变小鼠的行为分析显示,在一项探索性试验中,该突变与过度活跃有关。缺乏D3受体的纯合小鼠表现出增加的运动活动和饲养行为。 D3受体突变的杂合小鼠表现出相似的行为改变,尽管不太明显。我们的发现表明,D3受体在某些行为的控制中起抑制作用。

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