Ramalingam Pradeep, Poulos Michael G, Butler Jason M
Department of Medicine, Division of Regenerative Medicine, Ansary Stem Cell Institute, Weill Cornell Medical College, New York, USA.
Curr Opin Hematol. 2017 Jul;24(4):289-299. doi: 10.1097/MOH.0000000000000350.
Hematopoietic stem cells (HSCs) predominantly reside either in direct contact or in close proximity to the vascular endothelium throughout their lifespan. From the moment of HSC embryonic specification from hemogenic endothelium, endothelial cells (ECs) act as a critical cellular-hub that regulates a vast repertoire of biological processes crucial for HSC maintenance throughout its lifespan. In this review, we will discuss recent findings in endothelial niche-mediated regulation of HSC function during development, aging and regenerative conditions.
Studies employing genetic vascular models have unequivocally confirmed that ECs provide the essential instructive cues for HSC emergence during embryonic development as well as adult HSC maintenance during homeostasis and regeneration. Aging of ECs may impair their ability to maintain HSC function contributing to the development of aging-associated hematopoietic deficiencies. These findings have opened up new avenues to explore the therapeutic application of ECs. ECs can be adapted to serve as an instructive platform to expand bona fide HSCs and also utilized as a cellular therapy to promote regeneration of the hematopoietic system following myelosuppressive and myeloablative injuries.
ECs provide a fertile niche for maintenance of functional HSCs throughout their lifecycle. An improved understanding of the EC-HSC cross-talk will pave the way for development of EC-directed strategies for improving HSC function during aging.
造血干细胞(HSC)在其整个生命周期中主要直接接触或紧邻血管内皮细胞。从造血内皮细胞确定HSC胚胎特征的那一刻起,内皮细胞(EC)就作为一个关键的细胞枢纽,调节着对HSC在其整个生命周期中维持至关重要的大量生物学过程。在本综述中,我们将讨论内皮微环境在发育、衰老和再生条件下对HSC功能调节的最新研究发现。
采用基因血管模型的研究明确证实,内皮细胞在胚胎发育过程中为HSC的出现以及在稳态和再生过程中成年HSC的维持提供了必要的指导信号。内皮细胞的衰老可能会损害其维持HSC功能的能力,从而导致与衰老相关的造血缺陷的发生。这些发现为探索内皮细胞的治疗应用开辟了新途径。内皮细胞可被改造为一个指导平台,用于扩增真正的HSC,也可作为一种细胞疗法,促进骨髓抑制和清髓性损伤后造血系统的再生。
内皮细胞在整个生命周期中为功能性HSC的维持提供了一个有利的微环境。对内皮细胞与HSC相互作用的更好理解将为开发在衰老过程中改善HSC功能的内皮细胞导向策略铺平道路。