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白细胞介素-15 调节成年神经干细胞的增殖和自我更新。

Interleukin-15 regulates proliferation and self-renewal of adult neural stem cells.

机构信息

Functional and Systems Neurobiology Department, Cajal Institute (CSIC), Madrid, Spain.

出版信息

Mol Biol Cell. 2011 Jun 15;22(12):1960-70. doi: 10.1091/mbc.E11-01-0053. Epub 2011 Apr 20.

Abstract

The impact of inflammation is crucial for the regulation of the biology of neural stem cells (NSCs). Interleukin-15 (IL-15) appears as a likely candidate for regulating neurogenesis, based on its well-known mitogenic properties. We show here that NSCs of the subventricular zone (SVZ) express IL-15, which regulates NSC proliferation, as evidenced by the study of IL-15-/- mice and the effects of acute IL-15 administration, coupled to 5-bromo-2'-deoxyuridine/5-ethynyl-2'-deoxyuridine dual-pulse labeling. Moreover, IL-15 regulates NSC differentiation, its deficiency leading to an impaired generation of neuroblasts in the SVZ-rostral migratory stream axis, recoverable through the action of exogenous IL-15. IL-15 expressed in cultured NSCs is linked to self-renewal, proliferation, and differentiation. IL-15-/- NSCs presented deficient proliferation and self-renewal, as evidenced in proliferation and colony-forming assays and the analysis of cell cycle-regulatory proteins. Moreover, IL-15-deficient NSCs were more prone to differentiate than wild-type NSCs, not affecting the cell population balance. Lack of IL-15 led to a defective activation of the JAK/STAT and ERK pathways, key for the regulation of proliferation and differentiation of NSCs. The results show that IL-15 is a key regulator of neurogenesis in the adult and is essential to understanding diseases with an inflammatory component.

摘要

炎症的影响对于神经干细胞(NSCs)的生物学调节至关重要。白细胞介素-15(IL-15)因其众所周知的有丝分裂特性,似乎是调节神经发生的一个候选分子。我们在这里表明,侧脑室下区(SVZ)的 NSCs 表达 IL-15,它调节 NSC 的增殖,这一点可以从 IL-15-/- 小鼠的研究和急性 IL-15 给药的影响,以及 5-溴-2'-脱氧尿苷/5-乙炔-2'-脱氧尿苷双脉冲标记中得到证实。此外,IL-15 还调节 NSC 的分化,其缺乏导致 SVZ-额状迁移流轴中的神经母细胞生成受损,可通过外源性 IL-15 的作用得到恢复。培养的 NSCs 中表达的 IL-15 与自我更新、增殖和分化有关。IL-15-/- NSCs 的增殖和自我更新能力受损,这可以从增殖和集落形成实验以及细胞周期调节蛋白的分析中得到证实。此外,与野生型 NSCs 相比,IL-15 缺陷型 NSCs 更容易分化,而不会影响细胞群体的平衡。缺乏 IL-15 导致 JAK/STAT 和 ERK 通路的激活缺陷,这是调节 NSCs 增殖和分化的关键。研究结果表明,IL-15 是成年神经发生的关键调节因子,对于理解具有炎症成分的疾病至关重要。

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