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与小鼠相比,成年大鼠海马体中新生神经元数量更多、成熟更快且更多地参与行为活动。

Adult-born hippocampal neurons are more numerous, faster maturing, and more involved in behavior in rats than in mice.

作者信息

Snyder Jason S, Choe Jessica S, Clifford Meredith A, Jeurling Sara I, Hurley Patrick, Brown Ashly, Kamhi J Frances, Cameron Heather A

机构信息

Unit on Neuroplasticity, National Institute of Mental Health, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Neurosci. 2009 Nov 18;29(46):14484-95. doi: 10.1523/JNEUROSCI.1768-09.2009.

Abstract

Neurons are born throughout adulthood in the hippocampus and show enhanced plasticity compared with mature neurons. However, there are conflicting reports on whether or not young neurons contribute to performance in behavioral tasks, and there is no clear relationship between the timing of maturation of young neurons and the duration of neurogenesis reduction in studies showing behavioral deficits. We asked whether these discrepancies could reflect differences in the properties of young neurons in mice and rats. We report that young neurons in adult rats show a mature neuronal marker profile and activity-induced immediate early gene expression 1-2 weeks earlier than those in mice. They are also twice as likely to escape cell death, and are 10 times more likely to be recruited into learning circuits. This comparison holds true in two different strains of mice, both of which show high rates of neurogenesis relative to other background strains. Differences in adult neurogenesis are not limited to the hippocampus, as the density of new neocortical neurons was 5 times greater in rats than in mice. Finally, in a test of function, we find that the contribution of young neurons to fear memory is much greater in rats than in mice. These results reveal substantial differences in new neuron plasticity and function between these two commonly studied rodent species.

摘要

神经元在成年期的整个过程中都在海马体中生成,并且与成熟神经元相比表现出更强的可塑性。然而,关于年轻神经元是否对行为任务的表现有贡献,存在相互矛盾的报道,而且在显示行为缺陷的研究中,年轻神经元的成熟时间与神经发生减少的持续时间之间没有明确的关系。我们询问这些差异是否可能反映了小鼠和大鼠中年轻神经元特性的不同。我们报告称,成年大鼠中的年轻神经元比小鼠中的年轻神经元提前1 - 2周呈现成熟神经元标志物谱和活动诱导的立即早期基因表达。它们逃避细胞死亡的可能性也是小鼠的两倍,被招募到学习回路中的可能性是小鼠的10倍。这种比较在两种不同品系的小鼠中也成立,这两种小鼠相对于其他背景品系都表现出较高的神经发生速率。成年神经发生的差异并不局限于海马体,因为大鼠中新皮质神经元的密度是小鼠的5倍。最后,在一项功能测试中,我们发现年轻神经元对恐惧记忆的贡献在大鼠中比在小鼠中要大得多。这些结果揭示了这两种常用实验啮齿动物物种在新神经元可塑性和功能方面的显著差异。

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