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构建能够维持未分化人脐带血造血干细胞和祖细胞的完全人源化且血管化的三维骨髓龛。

Engineering of fully humanized and vascularized 3D bone marrow niches sustaining undifferentiated human cord blood hematopoietic stem and progenitor cells.

作者信息

Born Gordian, Nikolova Marina, Scherberich Arnaud, Treutlein Barbara, García-García Andrés, Martin Ivan

机构信息

Department of Biomedicine, University Hospital Basel, University of Basel, Basel, Switzerland.

Department of Biomedical Engineering, University of Basel, Allschwill, Switzerland.

出版信息

J Tissue Eng. 2021 Sep 29;12:20417314211044855. doi: 10.1177/20417314211044855. eCollection 2021 Jan-Dec.

DOI:10.1177/20417314211044855
PMID:34616539
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8488506/
Abstract

Hematopoietic stem and progenitor cells (HSPCs) are frequently located around the bone marrow (BM) vasculature. These so-called perivascular niches regulate HSC function both in health and disease, but they have been poorly studied in humans due to the scarcity of models integrating complete human vascular structures. Herein, we propose the stromal vascular fraction (SVF) derived from human adipose tissue as a cell source to vascularize 3D osteoblastic BM niches engineered in perfusion bioreactors. We show that SVF cells form self-assembled capillary structures, composed by endothelial and perivascular cells, that add to the osteogenic matrix secreted by BM mesenchymal stromal cells in these engineered niches. In comparison to avascular osteoblastic niches, vascularized BM niches better maintain immunophenotypically-defined cord blood (CB) HSCs without affecting cell proliferation. In contrast, HSPCs cultured in vascularized BM niches showed increased CFU-granulocyte-erythrocyte-monocyte-megakaryocyte (CFU-GEMM) numbers. The vascularization also contributed to better preserve osteogenic gene expression in the niche, demonstrating that niche vascularization has an influence on both hematopoietic and stromal compartments. In summary, we have engineered a fully humanized and vascularized 3D BM tissue to model native human endosteal perivascular niches and revealed functional implications of this vascularization in sustaining undifferentiated CB HSPCs. This system provides a unique modular platform to explore hemato-vascular interactions in human healthy/pathological hematopoiesis.

摘要

造血干细胞和祖细胞(HSPCs)常位于骨髓(BM)脉管系统周围。这些所谓的血管周围微环境在健康和疾病状态下均调节造血干细胞功能,但由于缺乏整合完整人类血管结构的模型,它们在人类中的研究较少。在此,我们提出将源自人类脂肪组织的基质血管成分(SVF)作为一种细胞来源,用于使灌注生物反应器中构建的三维成骨骨髓微环境血管化。我们发现,SVF细胞形成由内皮细胞和血管周围细胞组成的自组装毛细血管结构,这些结构添加到这些工程化微环境中骨髓间充质基质细胞分泌的成骨基质中。与无血管的成骨微环境相比,血管化的骨髓微环境能更好地维持免疫表型定义的脐血(CB)造血干细胞,且不影响细胞增殖。相反,在血管化骨髓微环境中培养的造血干细胞显示集落形成单位 - 粒细胞 - 红细胞 - 单核细胞 - 巨核细胞(CFU - GEMM)数量增加。血管化还有助于更好地保留微环境中的成骨基因表达,表明微环境血管化对造血和基质区室均有影响。总之,我们构建了一个完全人源化且血管化的三维骨髓组织,以模拟天然人类骨内膜血管周围微环境,并揭示了这种血管化在维持未分化CB造血干细胞方面的功能意义。该系统提供了一个独特的模块化平台,用于探索人类健康/病理造血过程中的血液 - 血管相互作用。

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