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成年大脑中双皮质素的表达水平反映神经发生。

Doublecortin expression levels in adult brain reflect neurogenesis.

作者信息

Couillard-Despres Sebastien, Winner Beate, Schaubeck Susanne, Aigner Robert, Vroemen Maurice, Weidner Norbert, Bogdahn Ulrich, Winkler Jürgen, Kuhn Hans-Georg, Aigner Ludwig

机构信息

Volkswagen-Foundation Junior Group, University of Regensburg, Franz-Josef-Strauss Allee 11, 93053 Regensburg, Germany.

出版信息

Eur J Neurosci. 2005 Jan;21(1):1-14. doi: 10.1111/j.1460-9568.2004.03813.x.

Abstract

Progress in the field of neurogenesis is currently limited by the lack of tools enabling fast and quantitative analysis of neurogenesis in the adult brain. Doublecortin (DCX) has recently been used as a marker for neurogenesis. However, it was not clear whether DCX could be used to assess modulations occurring in the rate of neurogenesis in the adult mammalian central nervous system following lesioning or stimulatory factors. Using two paradigms increasing neurogenesis levels (physical activity and epileptic seizures), we demonstrate that quantification of DCX-expressing cells allows for an accurate measurement of modulations in the rate of adult neurogenesis. Importantly, we excluded induction of DCX expression during physiological or reactive gliogenesis and excluded also DCX re-expression during regenerative axonal growth. Our data validate DCX as a reliable and specific marker that reflects levels of adult neurogenesis and its modulation. We demonstrate that DCX is a valuable alternative to techniques currently used to measure the levels of neurogenesis. Importantly, in contrast to conventional techniques, analysis of neurogenesis through the detection of DCX does not require in vivo labelling of proliferating cells, thereby opening new avenues for the study of human neurogenesis under normal and pathological conditions.

摘要

神经发生领域的进展目前受到限制,因为缺乏能够快速、定量分析成年大脑中神经发生的工具。双皮质素(DCX)最近被用作神经发生的标志物。然而,尚不清楚DCX是否可用于评估成年哺乳动物中枢神经系统在损伤或刺激因素后神经发生速率的变化。我们使用两种增加神经发生水平的范例(体育活动和癫痫发作),证明对表达DCX的细胞进行定量可准确测量成年神经发生速率的变化。重要的是,我们排除了生理或反应性胶质细胞生成过程中DCX表达的诱导,也排除了再生轴突生长过程中DCX的重新表达。我们的数据验证了DCX是一种可靠且特异的标志物,可反映成年神经发生的水平及其调节。我们证明DCX是目前用于测量神经发生水平的技术的一种有价值的替代方法。重要的是,与传统技术不同,通过检测DCX分析神经发生不需要对增殖细胞进行体内标记,从而为在正常和病理条件下研究人类神经发生开辟了新途径。

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