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杂合型 DAT-Cre 小鼠中行为、药物反应和多巴胺转运体表达的性别依赖性改变。

Sex-dependent alterations in behavior, drug responses and dopamine transporter expression in heterozygous DAT-Cre mice.

机构信息

Institute of Neurophysiology, Goethe-University Frankfurt, Theodor-Stern-Kai 7, 60596, Frankfurt am Main, Germany.

National Institute on Drug Abuse Intramural Research Program, National Institutes of Health, 251 Bayview Blvd, Baltimore, MD, 21224, USA.

出版信息

Sci Rep. 2021 Feb 8;11(1):3334. doi: 10.1038/s41598-021-82600-x.

Abstract

Heterozygous mice that express Cre-recombinase under the dopamine transporter promoter (DAT-Cre knock in mice, or KI) are widely used for targeting midbrain dopamine neurons, under the assumption that their constitutive physiology is not affected. We report here that these mice display striking sex-dependent behavioral and molecular differences in relation to wildtypes (WT). Male and female KI mice were constitutively hyperactive, and male KI mice showed attenuated hyperlocomotor responses to amphetamine. In contrast, female KIs displayed a marked reduction in locomotion ("calming" effect) in response to the same dose of amphetamine. Furthermore, male and female DAT-Cre KI mice showed opposing differences in reinforcement learning, with females showing faster conditioning and males showing slower extinction. Other behavioral variables, including working memory and novelty preference, were not changed compared to WT. These effects were paralleled by differences in striatal DAT expression that disproportionately affected female KI mice. Our findings reveal clear limitations of the DAT-Cre line that must be considered when using this model.

摘要

在多巴胺转运蛋白启动子(DAT-Cre 敲入小鼠或 KI)下表达 Cre 重组酶的杂合子小鼠被广泛用于靶向中脑多巴胺神经元,假设它们的组成生理不受影响。我们在这里报告说,这些小鼠在行为和分子方面表现出显著的性别依赖性差异,与野生型(WT)相比。雄性和雌性 KI 小鼠持续表现出过度活跃,雄性 KI 小鼠对安非他命的过度运动反应减弱。相比之下,女性 KI 对相同剂量的安非他命表现出明显的运动减少(“镇静”作用)。此外,雄性和雌性 DAT-Cre KI 小鼠在强化学习方面表现出相反的差异,雌性表现出更快的条件作用,而雄性表现出较慢的消退。与 WT 相比,其他行为变量,包括工作记忆和新奇偏好,没有改变。这些影响与纹状体 DAT 表达的差异平行,这些差异不成比例地影响雌性 KI 小鼠。我们的发现揭示了 DAT-Cre 系的明显局限性,在使用该模型时必须考虑这些局限性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2872/7870653/4c4bbb8dc3ef/41598_2021_82600_Fig1_HTML.jpg

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