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本文引用的文献

1
Phylogenetic variation in cortical layer II immature neuron reservoir of mammals.哺乳动物皮质层 II 未成熟神经元库的系统发育变异。
Elife. 2020 Jul 21;9:e55456. doi: 10.7554/eLife.55456.
2
Brain Structural Plasticity: From Adult Neurogenesis to Immature Neurons.脑结构可塑性:从成人神经发生到未成熟神经元
Front Neurosci. 2020 Feb 4;14:75. doi: 10.3389/fnins.2020.00075. eCollection 2020.
3
Dynamic Changes in the Neurogenic Potential in the Ventricular-Subventricular Zone of Common Marmoset during Postnatal Brain Development.在普通狨猴出生后脑发育过程中,脑室-室下区的神经发生潜能的动态变化。
Cereb Cortex. 2020 Jun 1;30(7):4092-4109. doi: 10.1093/cercor/bhaa031.
4
No DCX-positive neurogenesis in the cerebral cortex of the adult primate.成年灵长类动物大脑皮层中不存在双皮质素(DCX)阳性神经发生。
Neural Regen Res. 2020 Jul;15(7):1290-1299. doi: 10.4103/1673-5374.272610.
5
Unraveling human adult hippocampal neurogenesis.解析人类成年海马神经发生。
Nat Protoc. 2020 Feb;15(2):668-693. doi: 10.1038/s41596-019-0267-y. Epub 2020 Jan 8.
6
Expression of progenitor cell/immature neuron markers does not present definitive evidence for adult neurogenesis.祖细胞/未成熟神经元标志物的表达并不能提供成年神经发生的确凿证据。
Mol Brain. 2019 Dec 10;12(1):108. doi: 10.1186/s13041-019-0522-8.
7
Analysis of proliferating neuronal progenitors and immature neurons in the human hippocampus surgically removed from control and epileptic patients.分析手术切除的正常人及癫痫患者的人海马中的增殖神经前体细胞和未成熟神经元。
Sci Rep. 2019 Dec 3;9(1):18194. doi: 10.1038/s41598-019-54684-z.
8
Functional Integration of Neuronal Precursors in the Adult Murine Piriform Cortex.成年鼠梨状皮层神经元前体细胞的功能整合。
Cereb Cortex. 2020 Mar 14;30(3):1499-1515. doi: 10.1093/cercor/bhz181.
9
Fluoxetine-induced dematuration of hippocampal neurons and adult cortical neurogenesis in the common marmoset.氟西汀诱导的食蟹猴海马神经元和成年皮质神经发生的成熟障碍。
Mol Brain. 2019 Aug 5;12(1):69. doi: 10.1186/s13041-019-0489-5.
10
Immature excitatory neurons develop during adolescence in the human amygdala.在人类杏仁核中,不成熟的兴奋性神经元在青春期发育。
Nat Commun. 2019 Jun 21;10(1):2748. doi: 10.1038/s41467-019-10765-1.

成人和儿童的阳性对照实验表明,成年人类海马体中几乎没有(如果有的话)新神经元产生。

Positive Controls in Adults and Children Support That Very Few, If Any, New Neurons Are Born in the Adult Human Hippocampus.

机构信息

Department of Neuroscience, University of Pittsburgh, Pittsburgh, Pennsylvania 15260.

Department of Neurology, University of California San Francisco, San Francisco, California 94143.

出版信息

J Neurosci. 2021 Mar 24;41(12):2554-2565. doi: 10.1523/JNEUROSCI.0676-20.2020.

DOI:10.1523/JNEUROSCI.0676-20.2020
PMID:33762407
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8018729/
Abstract

Adult hippocampal neurogenesis was originally discovered in rodents. Subsequent studies identified the adult neural stem cells and found important links between adult neurogenesis and plasticity, behavior, and disease. However, whether new neurons are produced in the human dentate gyrus (DG) during healthy aging is still debated. We and others readily observe proliferating neural progenitors in the infant hippocampus near immature cells expressing doublecortin (DCX), but the number of such cells decreases in children and few, if any, are present in adults. Recent investigations using dual antigen retrieval find many cells stained by DCX antibodies in adult human DG. This has been interpreted as evidence for high rates of adult neurogenesis, even at older ages. However, most of these DCX-labeled cells have mature morphology. Furthermore, studies in the adult human DG have not found a germinal region containing dividing progenitor cells. In this Dual Perspectives article, we show that dual antigen retrieval is not required for the detection of DCX in multiple human brain regions of infants or adults. We review prior studies and present new data showing that DCX is not uniquely expressed by newly born neurons: DCX is present in adult amygdala, entorhinal and parahippocampal cortex neurons despite being absent in the neighboring DG. Analysis of available RNA-sequencing datasets supports the view that DG neurogenesis is rare or absent in the adult human brain. To resolve the conflicting interpretations in humans, it is necessary to identify and visualize dividing neuronal precursors or develop new methods to evaluate the age of a neuron at the single-cell level.

摘要

成人海马神经发生最初在啮齿动物中被发现。随后的研究确定了成人神经干细胞,并发现了成人神经发生与可塑性、行为和疾病之间的重要联系。然而,在健康衰老过程中,人类齿状回(DG)是否产生新的神经元仍存在争议。我们和其他人在靠近表达双皮质素(DCX)的未成熟细胞的婴儿海马中很容易观察到增殖的神经祖细胞,但这些细胞的数量在儿童中减少,在成年人中几乎不存在。最近使用双重抗原检索的研究发现,成年人类 DG 中有许多细胞被 DCX 抗体染色。这被解释为成人神经发生率很高的证据,即使在年龄较大时也是如此。然而,这些 DCX 标记的细胞大多具有成熟的形态。此外,对成年人类 DG 的研究并未发现含有分裂祖细胞的生殖区。在这篇双视角文章中,我们表明,双重抗原检索不是检测婴儿或成人多个大脑区域 DCX 的必需条件。我们回顾了先前的研究,并提出了新的数据,表明 DCX 并非新生神经元所特有表达:尽管在相邻的 DG 中不存在,但 DCX 存在于成年杏仁核、内嗅皮质和海马旁皮质神经元中。对现有 RNA 测序数据集的分析支持 DG 神经发生在成人脑中罕见或不存在的观点。为了解决人类中相互矛盾的解释,有必要识别和可视化分裂的神经元前体,或开发新的方法在单细胞水平评估神经元的年龄。