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Human adult neurogenesis across the ages: An immunohistochemical study

机译:各个年龄段的人类成人神经发生:一项免疫组织化学研究

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Aims: Neurogenesis in the postnatal human brain occurs in two neurogenic niches; the subventricular zone (SVZ) in the wall of the lateral ventricles and the subgranular zone (SGZ) of the hippocampus. The extent to which this physiological process continues into adulthood is an area of ongoing research. This study aimed to characterize markers of cell proliferation and assess the efficacy of antibodies used to identify neurogenesis in both neurogenic niches of the human brain. Methods: Cell proliferation and neurogenesis were simultaneously examined in the SVZ and SGZ of 23 individuals aged 0.2-59 years, using immunohistochemistry and immunofluorescence in combination with unbiased stereology. Results: There was a marked decline in proliferating cells in both neurogenic niches in early infancy with levels reaching those seen in the adjacent parenchyma by 4 and 1 year of age, in the SVZ and SGZ, respectively. Furthermore, the phenotype of these proliferating cells in both niches changed with age. In infants, proliferating cells co-expressed neural progenitor (epidermal growth factor receptor), immature neuronal (doublecortin and beta III tubulin) and oligodendrocytic (Olig2) markers. However, after 3 years of age, microglia were the only proliferating cells found in either niche or in the adjacent parenchyma. Conclusions: This study demonstrates a marked decline in neurogenesis in both neurogenic niches in early childhood, and that the sparse proliferating cells in the adult brain are largely microglia.
机译:目的:产后人脑中的神经发生发生在两个神经源性壁ches中。侧脑室壁的脑室下区域(SVZ)和海马的颗粒下区域(SGZ)。这种生理过程持续到成年的程度是一个正在进行的研究领域。这项研究旨在表征细胞增殖的标志物,并评估用于鉴定人脑两个神经源利基神经元的抗体的功效。方法:采用免疫组织化学和免疫荧光技术结合无偏见的立体影像学方法,同时检测了23位0.2-59岁个体的SVZ和SGZ细胞的增殖和神经发生。结果:婴儿早期两个神经源性壁ni的增生细胞均明显下降,到SVZ和SGZ分别达到4岁和1岁时在邻近实质中所见的水平。此外,两个小生境中这些增殖细胞的表型随年龄变化。在婴儿中,增殖细胞共表达神经祖细胞(表皮生长因子受体),神经元未成熟(双皮质素和βIII微管蛋白)和少突胶质细胞(Olig2)标记。但是,在3岁以后,小胶质细胞是在利基或邻近薄壁组织中发现的唯一增殖细胞。结论:这项研究表明,儿童早期两个神经源性利基神经元的发生均显着下降,并且成年大脑中稀疏的增殖细胞主要是小胶质细胞。

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