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胚胎期和成年期中风模型中细胞周期动力学的联系:一种分析方法。

Linkage of cell cycle kinetics between embryonic and adult stroke models: an analytical approach.

作者信息

Lu Mei, Zhang Rui Lan, Zhang Zheng Gang, Yang James J, Chopp Michael

机构信息

Department of Biostatistics and Research Epidemiology, Henry Ford Health Sciences Center, One Ford Place, Ste. 3E, Detroit, MI 48202, USA.

出版信息

J Neurosci Methods. 2007 Apr 15;161(2):323-30. doi: 10.1016/j.jneumeth.2006.10.021. Epub 2006 Dec 4.

Abstract

In the adult brain, neurogenesis occurs in the subventricular zone (SVZ) of the lateral ventricle. The proliferating population and the cell cycle kinetics in the ventricular zone regulate cortical neurogenesis during the development. Using the embryonic model, we investigated kinetics of SVZ cells in adult rats after stroke, incorporating migration of SVZ cells to the ischemic boundary. Concurrent linear regressions were considered through iteration to improve precision of parameter estimation. We found no model-fit difference in stroke with and without the migration (p=0.31), suggesting no migration effect on assessment of the cell kinetics. Stroke increased SVZ cell proliferation (20% in non-stroke and 31% in stroke p<0.01). Cell cycle durations in stroke were reduced for the total cycle length (19h for non-stroke and 15.3h for stroke, p<0.05), in G1 phase (12.6 h for non-stroke and 9.6 h for stroke, p<0.01), but were the same in S, M2, and in G2 phases compared to non-stroke, indicating that stroke reduces the total cell cycle length, specially in G1 phase. We conclude that cell cycle kinetic models for cortical development can be adapted to the kinetics of adult SVZ cells after stroke. The analytical approach may be useful for studying neural progenitor cell proliferation under different treatments.

摘要

在成人大脑中,神经发生发生在侧脑室的室下区(SVZ)。在发育过程中,脑室区的增殖群体和细胞周期动力学调节着皮质神经发生。利用胚胎模型,我们研究了成年大鼠中风后SVZ细胞的动力学,包括SVZ细胞向缺血边界的迁移。通过迭代考虑并发线性回归以提高参数估计的精度。我们发现有迁移和无迁移的中风模型拟合没有差异(p = 0.31),表明迁移对细胞动力学评估没有影响。中风增加了SVZ细胞增殖(非中风组为20%,中风组为31%,p < 0.01)。中风时细胞周期持续时间在总周期长度上缩短(非中风组为19小时,中风组为15.3小时,p < 0.05),在G1期(非中风组为12.6小时,中风组为9.6小时,p < 0.01),但与非中风组相比,S期、M2期和G2期相同,表明中风缩短了总细胞周期长度,特别是在G1期。我们得出结论,皮质发育的细胞周期动力学模型可以适用于成年大鼠中风后SVZ细胞的动力学。该分析方法可能有助于研究不同处理下神经祖细胞的增殖。

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