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Novelty-seeking behavior predicts vulnerability in a rodent model of depression.寻求新奇行为预测抑郁的啮齿动物模型中的脆弱性。
Physiol Behav. 2011 May 3;103(2):210-6. doi: 10.1016/j.physbeh.2011.02.001. Epub 2011 Feb 12.
2
Altered expression of glutamate signaling, growth factor, and glia genes in the locus coeruleus of patients with major depression.谷氨酸信号、生长因子和神经胶质基因在重度抑郁症患者蓝斑核中的表达改变。
Mol Psychiatry. 2011 Jun;16(6):634-46. doi: 10.1038/mp.2010.44. Epub 2010 Apr 13.
3
Postnatal development of the human hippocampal formation.人类海马结构的出生后发育。
Adv Anat Embryol Cell Biol. 2010;206:1-86.
4
Neural and environmental factors impacting maternal behavior differences in high- versus low-novelty-seeking rats.影响高新奇寻求大鼠与低新奇寻求大鼠母性行为差异的神经和环境因素。
Horm Behav. 2010 Apr;57(4-5):463-73. doi: 10.1016/j.yhbeh.2010.02.004. Epub 2010 Feb 13.
5
An animal model of genetic vulnerability to behavioral disinhibition and responsiveness to reward-related cues: implications for addiction.遗传易感性导致行为抑制障碍和对奖励相关线索反应性的动物模型:对成瘾的影响。
Neuropsychopharmacology. 2010 Jan;35(2):388-400. doi: 10.1038/npp.2009.142.
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A new role for FGF2 as an endogenous inhibitor of anxiety.成纤维细胞生长因子2作为内源性焦虑抑制剂的新作用。
J Neurosci. 2009 May 13;29(19):6379-87. doi: 10.1523/JNEUROSCI.4829-08.2009.
7
Individual differences in the attribution of incentive salience to reward-related cues: Implications for addiction.奖励相关线索激励显著性归因中的个体差异:对成瘾的影响。
Neuropharmacology. 2009;56 Suppl 1(Suppl 1):139-48. doi: 10.1016/j.neuropharm.2008.06.027. Epub 2008 Jun 21.
8
The effects of novelty-seeking phenotypes and sex differences on acquisition of cocaine self-administration in selectively bred High-Responder and Low-Responder rats.新奇寻求表型和性别差异对选择性培育的高反应性和低反应性大鼠可卡因自我给药习得的影响。
Pharmacol Biochem Behav. 2008 Sep;90(3):331-8. doi: 10.1016/j.pbb.2008.03.008. Epub 2008 Mar 25.
9
Environmental novelty is signaled by reduction of the hippocampal theta frequency.海马体θ波频率降低表明环境出现新变化。
Hippocampus. 2008;18(4):340-8. doi: 10.1002/hipo.20394.
10
Prenatal stress does not alter innate novelty-seeking behavioral traits, but differentially affects individual differences in neuroendocrine stress responsivity.产前应激不会改变天生的寻求新奇行为特征,但会不同程度地影响神经内分泌应激反应的个体差异。
Psychoneuroendocrinology. 2008 Feb;33(2):162-77. doi: 10.1016/j.psyneuen.2007.10.012.

啮齿动物寻求新奇和情绪反应差异的发展基础。

Developmental underpinnings of differences in rodent novelty-seeking and emotional reactivity.

机构信息

Department of Psychiatry and Behavioral Neurobiology, University of Alabama at Birmingham, 1720 7th Avenue South, SC 745 Birmingham, AL 35233, USA.

出版信息

Eur J Neurosci. 2011 Sep;34(6):994-1005. doi: 10.1111/j.1460-9568.2011.07811.x. Epub 2011 Aug 22.

DOI:10.1111/j.1460-9568.2011.07811.x
PMID:21864320
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3310433/
Abstract

Innate differences in human temperament strongly influence how individuals cope with stress and also predispose towards specific types of psychopathology. The present study examines the developing brain in an animal model of temperamental differences to examine how altered neurodevelopment may engender differences in emotional reactivity that are stable throughout the animal's life. We utilize selectively-bred High Responder (bHR) and Low Responder (bLR) rats that exhibit dramatic emotional behavior differences, with bHRs exhibiting exaggerated novelty-exploration, aggression, impulsivity and drug self-administration, and bLRs showing marked behavioral inhibition and exaggerated anxiety-like and depressive-like behavior. Using Affymetrix microarrays, we assessed bLR and bHR gene expression in the developing brain on postnatal days (P)7, 14 and 21, focusing on the hippocampus and nucleus accumbens, two regions related to emotionality and known to differ in adult bLR and bHR rats. We found dramatic gene expression differences between bLR and bHR in the P7 and P14 hippocampus, with minimal differences in the nucleus accumbens. Some of the most profound differences involved genes critical for neurodevelopment and synaptogenesis. Stereological studies evaluated hippocampal structure in developing bHR and bLR pups, revealing enhanced hippocampal volume and cell proliferation in bLR animals. Finally, behavioral studies showed that the characteristic bHR and bLR behavioral phenotypes emerge very early in life, with exploratory differences apparent at P16 and anxiety differences present by P25. Together these data point to specific brain regions and critical periods when the bHR and bLR phenotypes begin to diverge, which may eventually allow us to test possible therapeutic interventions to normalize extreme phenotypes (e.g. the anxiety-prone nature of bLRs or drug addiction proclivity of bHRs).

摘要

人类气质的先天差异强烈影响个体如何应对压力,也使个体容易产生特定类型的精神病理学。本研究在气质差异的动物模型中研究发育中的大脑,以检查神经发育的改变如何产生贯穿动物一生的稳定情绪反应差异。我们利用选择性繁殖的高反应(bHR)和低反应(bLR)大鼠,这些大鼠表现出明显的情绪行为差异,bHR 表现出夸张的新奇探索、攻击性、冲动性和药物自我给药,而 bLR 则表现出明显的行为抑制和夸张的焦虑样和抑郁样行为。使用 Affymetrix 微阵列,我们评估了发育中的大脑在出生后第 7、14 和 21 天的 bLR 和 bHR 基因表达,重点是海马体和伏隔核,这两个区域与情绪有关,已知在成年 bLR 和 bHR 大鼠中存在差异。我们发现 bLR 和 bHR 在 P7 和 P14 海马体中的基因表达存在显著差异,而在伏隔核中的差异很小。一些最显著的差异涉及神经发育和突触发生的关键基因。立体学研究评估了发育中的 bHR 和 bLR 幼崽的海马体结构,发现 bLR 动物的海马体体积和细胞增殖增强。最后,行为研究表明,bHR 和 bLR 的特征行为表型在生命早期就出现了,在 P16 时出现探索性差异,在 P25 时出现焦虑差异。这些数据共同指向特定的大脑区域和关键时期,bHR 和 bLR 表型开始出现分歧,这最终可能使我们能够测试可能的治疗干预措施,使极端表型正常化(例如 bLR 的焦虑倾向或 bHR 的药物成瘾倾向)。