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拉托菲林-3 杂合突变与 Sprague Dawley 大鼠纯合突变:对自我中心和客体中心记忆及运动活动的影响。

Latrophilin-3 heterozygous versus homozygous mutations in Sprague Dawley rats: Effects on egocentric and allocentric memory and locomotor activity.

机构信息

Department of Pediatrics, University of Cincinnati College of Medicine and Division of Neurology, Cincinnati Children's Research Foundation, Cincinnati, Ohio, USA.

Department of Human Genetics, University of Michigan Medical Center, Ann Arbor, Michigan, USA.

出版信息

Genes Brain Behav. 2022 Sep;21(7):e12817. doi: 10.1111/gbb.12817. Epub 2022 Aug 19.

Abstract

Latrophilin-3 (LPHN3) is a brain specific G-protein coupled receptor associated with increased risk of attention deficit hyperactivity disorder (ADHD) and cognitive deficits. CRISPR/Cas9 was used to generate a constitutive knockout (KO) rat of Lphn3 by deleting exon 3, based on human data that LPHN3 variants are associated with some cases of ADHD. Lphn3 KO rats are hyperactive with an attenuated response to ADHD medication and have cognitive deficits. Here, we tested KO, heterozygous (HET), and wildtype (WT) rats to determine if there was a gene-dosage effect. We tested the rats in home-cage activity starting at postnatal day (P)35 and P50, followed by tests of egocentric learning (Cincinnati water maze [CWM]), spatial learning (Morris water maze [MWM]), working memory (radial water maze [RWM]), incidental learning (novel object recognition [NOR]), acoustic startle response (ASR) habituation, tactile startle response (TSR) habituation, prepulse modification of acoustic startle, shuttle-box passive avoidance, conditioned freezing, and a mirror image version of the CWM. KO and HET rats were hyperactive. KO and HET rats had egocentric (CWM) and spatial deficits (MWM), increased startle response, and KO rats showed less conditioned freezing on contextual and cued memory; there were no effects on working memory (RWM) or passive avoidance. The selective gene-dosage effect in Lphn3 HET rats indicates that Lphn3 exhibits dominate expression on functions where it is most abundantly expressed (striatum, hippocampus) but not on behaviors mediated by regions of low expression. The data add further evidence to the impact of this synaptic protein on brain function and behavior.

摘要

拉普罗林-3(LPHN3)是一种与注意力缺陷多动障碍(ADHD)风险增加和认知缺陷相关的脑特异性 G 蛋白偶联受体。基于人类数据,即 LPHN3 变体与一些 ADHD 病例有关,我们使用 CRISPR/Cas9 技术生成了 Lphn3 的组成型敲除(KO)大鼠,该方法通过删除外显子 3 来实现。Lphn3 KO 大鼠表现出过度活跃,对 ADHD 药物的反应减弱,并且存在认知缺陷。在这里,我们测试了 KO、杂合子(HET)和野生型(WT)大鼠,以确定是否存在基因剂量效应。我们在出生后第 35 天和第 50 天开始在大鼠的笼内活动中对它们进行测试,随后进行自我中心学习(辛辛那提水迷宫 [CWM])、空间学习(Morris 水迷宫 [MWM])、工作记忆(放射状水迷宫 [RWM])、偶然学习(新物体识别 [NOR])、听觉惊跳反应(ASR)习惯化、触觉惊跳反应(TSR)习惯化、听觉惊跳的预备脉冲调制、穿梭箱被动回避、条件性冻僵,以及 CWM 的镜像版本。KO 和 HET 大鼠表现出过度活跃。KO 和 HET 大鼠的自我中心(CWM)和空间缺陷(MWM)、惊跳反应增加,以及 KO 大鼠在情境和提示记忆的条件性冻僵中表现出较少的反应;对工作记忆(RWM)或被动回避没有影响。Lphn3 HET 大鼠中存在的选择性基因剂量效应表明,Lphn3 在其表达最丰富的区域(纹状体、海马体)上表现出显性表达,而在表达水平较低的区域介导的行为上则没有表现出这种作用。这些数据为这种突触蛋白对大脑功能和行为的影响提供了进一步的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5332/9744505/f05eb4696a18/GBB-21-e12817-g002.jpg

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