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造血骨髓微环境生态系统。

The Hematopoietic Bone Marrow Niche Ecosystem.

作者信息

Fröbel Julia, Landspersky Theresa, Percin Gülce, Schreck Christina, Rahmig Susann, Ori Alessandro, Nowak Daniel, Essers Marieke, Waskow Claudia, Oostendorp Robert A J

机构信息

Immunology of Aging, Leibniz Institute on Aging - Fritz Lipmann Institute, Jena, Germany.

School of Medicine, Department of Internal Medicine III, Technical University of Munich, Munich, Germany.

出版信息

Front Cell Dev Biol. 2021 Jul 22;9:705410. doi: 10.3389/fcell.2021.705410. eCollection 2021.

Abstract

The bone marrow (BM) microenvironment, also called the BM niche, is essential for the maintenance of fully functional blood cell formation (hematopoiesis) throughout life. Under physiologic conditions the niche protects hematopoietic stem cells (HSCs) from sustained or overstimulation. Acute or chronic stress deregulates hematopoiesis and some of these alterations occur indirectly via the niche. Effects on niche cells include skewing of its cellular composition, specific localization and molecular signals that differentially regulate the function of HSCs and their progeny. Importantly, while acute insults display only transient effects, repeated or chronic insults lead to sustained alterations of the niche, resulting in HSC deregulation. We here describe how changes in BM niche composition (ecosystem) and structure (remodeling) modulate activation of HSCs . Current knowledge has revealed that upon chronic stimulation, BM remodeling is more extensive and otherwise quiescent HSCs may be lost due to diminished cellular maintenance processes, such as autophagy, ER stress response, and DNA repair. Features of aging in the BM ecology may be the consequence of intermittent stress responses, ultimately resulting in the degeneration of the supportive stem cell microenvironment. Both chronic stress and aging impair the functionality of HSCs and increase the overall susceptibility to development of diseases, including malignant transformation. To understand functional degeneration, an important prerequisite is to define distinguishing features of unperturbed niche homeostasis in different settings. A unique setting in this respect is xenotransplantation, in which human cells depend on niche factors produced by other species, some of which we will review. These insights should help to assess deviations from the steady state to actively protect and improve recovery of the niche ecosystem to optimally sustain healthy hematopoiesis in experimental and clinical settings.

摘要

骨髓(BM)微环境,也称为BM龛,对于维持一生中全功能血细胞生成(造血作用)至关重要。在生理条件下,龛保护造血干细胞(HSC)免受持续或过度刺激。急性或慢性应激会使造血作用失调,其中一些改变是通过龛间接发生的。对龛细胞的影响包括其细胞组成的偏差、特定定位和分子信号,这些信号会差异性地调节HSC及其子代的功能。重要的是,虽然急性损伤仅表现出短暂效应,但反复或慢性损伤会导致龛的持续改变,从而导致HSC失调。我们在此描述BM龛组成(生态系统)和结构(重塑)的变化如何调节HSC的激活。目前的知识表明,在慢性刺激下,BM重塑更为广泛,原本静止的HSC可能会因细胞维持过程(如自噬、内质网应激反应和DNA修复)减弱而丢失。BM生态老化的特征可能是间歇性应激反应的结果,最终导致支持性干细胞微环境的退化。慢性应激和衰老都会损害HSC的功能,并增加对包括恶性转化在内的疾病发展的总体易感性。为了理解功能退化,一个重要的前提是定义不同情况下未受干扰的龛稳态的显著特征。在这方面,一个独特的情况是异种移植,其中人类细胞依赖于其他物种产生的龛因子,我们将对其中一些进行综述。这些见解应有助于评估与稳态的偏差,以积极保护和改善龛生态系统的恢复,从而在实验和临床环境中最佳地维持健康的造血作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2985/8339972/b83f6a7a8d13/fcell-09-705410-g001.jpg

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