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Aging of the Niche and the Microenvironment and Its Role in Stem Cell Aging

机译:利基和微环境老化及其在干细胞老化中的作用

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Stem cell function declines with age in both humans and mice. It has been hypothesized that aging of stem cells is the underlying cause of impaired tissue homeostasis as well as cancer in aged individuals, which might ultimately limit the lifespan. In 1978, Schofield proposed the 'niche'hypothesis to describe the physiologically limited microenvironmentthat supports stem cells.This hypothesis has been confirmed in multiple stem cell systems from distinct organisms over the last decade and is currently an active field of research in stem cell biology. In recent years the effect of aging of the niche on altered phenotypes associated with aged stem cells has been more and more appreciated. One central question in stem cell aging research is consequently the identification of the contribution of stem cell intrinsic versus extrinsic factors (including the niche and/or systemic factors) to stem cell aging, which is critically important with respect to therapeutic interventions in light of reversion/ rejuvenation.Thefollowing chapter summarizes presentations from the 3rd Else Kroner-Fresenius Symposium on Molecular Mechanisms of Stem Cell Aging that focused primarily on elucidating alterations of stem cell-niche interactions, age-associated leukemia, and systemic influences on stem cell aging, both in Drosophila and mice, provided by Drs. Xie, Yamashita, Jones, DeGre-gori, and Geiger.
机译:干细胞功能随着人类和小鼠的年龄而下降。已经假设干细胞老化是组织稳态的潜在原因以及年龄患者的癌症,这可能最终限制了寿命。 1978年,斯科夫德提出了“地理位置”,以描述生理学上有限的微环境,支持干细胞。在过去十年中,在多种干细胞系统中已经在多种生物体中证实了这一假设,目前是干细胞生物学的有源研究领域。近年来,越来越多地欣赏了利用效力老化对与老年干细胞相关的改变表型的影响。因此,干细胞老化研究中的一个核心问题是鉴定干细胞内在因子(包括利基和/或系统因素)对干细胞老化的贡献,这对于逆转时,这对治疗性干预令人统治性重要/恢复活力。第三章综述了克里姆斯 - 弗雷斯妮乌斯的第3次母亲对干细胞老化的分子机制的演示,主要是阐明干细胞 - 利基相互作用,年龄相关的白血病和对干细胞老化的系统影响的改变,都在阐明Drs提供的果蝇和老鼠。谢,山脉,琼斯,侏儒和冰叶。

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