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V1 vasopressin receptor antisense oligodeoxynucleotide into septum reduces vasopressin binding, social discrimination abilities, and anxiety-related behavior in rats.将血管加压素 V1 受体反义寡脱氧核苷酸注入大鼠的中隔会降低血管加压素结合力、社会辨别能力以及与焦虑相关的行为。
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Viral vector-mediated gene transfer of the vole V1a vasopressin receptor in the rat septum: improved social discrimination and active social behaviour.病毒载体介导的田鼠V1a血管加压素受体基因导入大鼠隔膜:改善社会辨别能力和积极的社会行为。
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Vasopressin V1a, but not V1b, receptors within the PVN of lactating rats mediate maternal care and anxiety-related behaviour.哺乳期大鼠室旁核内的血管升压素V1a受体而非V1b受体介导母性行为和焦虑相关行为。
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Evidence for the existence of vasopressin V2 receptor mRNA in rat hippocampus.大鼠海马中血管加压素V2受体mRNA存在的证据。
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Arginine vasopressin-induced sensitization in brain: facilitated inositol phosphate production without changes in receptor number.精氨酸加压素诱导的脑致敏作用:肌醇磷酸生成增加而受体数量无变化。
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Differences in intermale aggression are accompanied by opposite vasopressin release patterns within the septum in rats bred for low and high anxiety.在为低焦虑和高焦虑培育的大鼠中,雄性间攻击性的差异伴随着隔区内血管加压素释放模式的相反变化。
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将血管加压素 V1 受体反义寡脱氧核苷酸注入大鼠的中隔会降低血管加压素结合力、社会辨别能力以及与焦虑相关的行为。

V1 vasopressin receptor antisense oligodeoxynucleotide into septum reduces vasopressin binding, social discrimination abilities, and anxiety-related behavior in rats.

作者信息

Landgraf R, Gerstberger R, Montkowski A, Probst J C, Wotjak C T, Holsboer F, Engelmann M

机构信息

Max Planck Institute of Psychiatry, Clinical Institute, Munich, Germany.

出版信息

J Neurosci. 1995 Jun;15(6):4250-8. doi: 10.1523/JNEUROSCI.15-06-04250.1995.

DOI:10.1523/JNEUROSCI.15-06-04250.1995
PMID:7790909
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6577715/
Abstract

To develop and validate a vasopressin (AVP) receptor knockdown strategy, we infused an antisense oligodeoxynucleotide to the V1 subtype mRNA into the septum of male rats with osmotic minipumps and measured behavioral, cellular and molecular parameters. Compared to vehicle and scrambled-sequence oligo controls, chronic antisense administration for up to 4 d diminished the ability of the animals to distinguish a previously exposed juvenile from a novel one and to respond to exogenous AVP (1 ng/5 microliters, intracerebroventricular) with an improved social memory. Furthermore, anxiety-related behavior was reduced. As measured in the behaviorally tested rats, antisense treatment resulted in a reduced binding of radiolabeled AVP in the septum, but not in other limbic brain areas (receptor autoradiography), and an increased amount of V1 receptor mRNA (reverse transcriptase PCR), indicating translational arrest and ongoing transcriptional activity. In sense oligo-treated rats, on the other hand, both the social and the anxiety-related behavior scores lay between levels obtained in control and antisense-treated animals. These sense-treated rats showed a slightly reduced V1 receptor density in the septum and reduced receptor mRNA levels, indicating hybridization of the sense oligo to the DNA. The data show the potential of antisense targeting to further reveal relationships between local gene expression, neuropeptide-receptor interactions in distinct brain areas, and behavioral performance.

摘要

为了开发并验证一种血管加压素(AVP)受体敲低策略,我们用渗透微型泵将针对V1亚型mRNA的反义寡脱氧核苷酸注入雄性大鼠的隔区,并测量行为、细胞和分子参数。与载体对照组和乱序寡核苷酸对照组相比,长达4天的慢性反义给药降低了动物区分先前接触过的幼崽和新幼崽的能力,以及对外源性血管加压素(1纳克/5微升,脑室内注射)做出反应并改善社交记忆的能力。此外,与焦虑相关的行为也有所减少。在经过行为测试的大鼠中,反义治疗导致隔区放射性标记血管加压素的结合减少,但在其他边缘脑区未出现这种情况(受体放射自显影),并且V1受体mRNA的量增加(逆转录聚合酶链反应),表明翻译停滞和转录活动持续进行。另一方面,在正义寡核苷酸处理的大鼠中,社交行为和与焦虑相关的行为评分均介于对照组和反义处理组动物所获得的水平之间。这些正义处理的大鼠在隔区的V1受体密度略有降低,受体mRNA水平也降低,表明正义寡核苷酸与DNA发生了杂交。数据显示了反义靶向在进一步揭示局部基因表达、不同脑区神经肽 - 受体相互作用与行为表现之间关系方面的潜力。