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神经血管信号提示了内源性干细胞沿着血管激活的传播机制。

Neurovascular signals suggest a propagation mechanism for endogenous stem cell activation along blood vessels.

机构信息

Department of Medicine, University of Dresden, Dresden, Germany.

出版信息

CNS Neurol Disord Drug Targets. 2012 Nov 1;11(7):805-17. doi: 10.2174/1871527311201070805.

Abstract

Stem cell-based therapies for central nervous system disorders are intensely pursued. Such approaches can be divided into two categories: Transplantation-based, and those that aim to pharmacologically target the endogenous stem cell population in the tissue. Endogenous stem cell - based strategies avoid the problem of immune incompatibility between the host and the grafted cells. They also avoid the placement of a large amount of cells in confined areas, a manipulation which alters the characteristics of the neurovascular microenvironment. We show here that massive pharmacological activation (increase in cell numbers) of the endogenous neural stem cell population in the adult rodent brain maintains the cytoarchitecture of the neurovascular niche. Distances between adjacent stem cells (identified by expression of Hes3) are maintained above a minimum. Hes3+ cells maintain their physical association with blood vessels. These results also suggest a mechanism by which the activation signal from the lateral ventricle can be propagated to areas a long distance away from the lateral ventricles, through autocrine/paracrine actions between adjacent Hes3+ cells, along blood vessels. Finally, powerful effects of angiopoietin 2 on Hes3+ cells help explain the prevalence of proliferating endogenous neural stem cells close to the subventricular zone (an area of high angiopoietin 2 concentration) and the quiescent state of stem cells away from the ventricles and their tight physical association with blood vessels (which express high levels of angiopoietin 1, a cytokine that opposes angiopoietin 2 functions).

摘要

针对中枢神经系统疾病的基于干细胞的疗法正在被深入研究。这些方法可以分为两类:基于移植的方法,以及旨在通过药理学手段靶向组织内内源性干细胞群体的方法。内源性干细胞为基础的策略避免了宿主与移植细胞之间免疫不相容的问题。它们还避免了将大量细胞放置在有限的区域内,这种操作改变了神经血管微环境的特性。我们在这里表明,成年啮齿动物大脑中内源性神经干细胞群体的大规模药理学激活(细胞数量增加)维持了神经血管壁龛的细胞结构。相邻干细胞(通过 Hes3 的表达来识别)之间的距离保持在最小值以上。Hes3+细胞保持与血管的物理联系。这些结果还表明了一种机制,即来自侧脑室的激活信号可以通过相邻 Hes3+细胞之间的自分泌/旁分泌作用,沿着血管,从侧脑室远距离传播到其他区域。最后,血管生成素 2 对 Hes3+细胞的强大作用有助于解释为什么增殖的内源性神经干细胞在靠近脑室下区(血管生成素 2 浓度高的区域)的地方很普遍,而远离脑室的干细胞处于静止状态,并且与血管紧密地物理联系(血管表达高水平的血管生成素 1,一种与血管生成素 2 功能相反的细胞因子)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/349a/3580829/7f40e23cd5fa/CDTCNSND-11-805_F1.jpg

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