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前瞻性分离龛中非造血细胞及其与 HSCs 的差异分子相互作用。

Prospective isolation of nonhematopoietic cells of the niche and their differential molecular interactions with HSCs.

机构信息

Regeneration in Hematopoiesis and Animal Models in Hematopoiesis, Institute for Immunology Medical Faculty, Technische Universität (TU) Dresden, Dresden, Germany.

Theoretical Systems Biology, German Cancer Research Center, Heidelberg, Germany.

出版信息

Blood. 2019 Oct 10;134(15):1214-1226. doi: 10.1182/blood.2019000176.

Abstract

A major limitation preventing in vivo modulation of hematopoietic stem cells (HSCs) is the incomplete understanding of the cellular and molecular support of the microenvironment in regulating HSC fate decisions. Consequently, murine HSCs cannot be generated, maintained, or expanded in culture over extended periods of time. A significantly improved understanding of the bone marrow niche environment and its molecular interactions with HSCs is pivotal to overcoming this challenge. We here prospectively isolated all major nonhematopoietic cellular niche components and cross-correlate them in detail with niche cells defined by lineage marking or tracing. Compiling an extensive database of soluble and membrane-bound ligand-receptor interactions, we developed a computational method to infer potential cell-to-cell interactions based on transcriptome data of sorter-purified niche cells and hematopoietic stem and progenitor cell subpopulations. Thus, we establish a compendium of the molecular communication between defined niche components and HSCs. Our analysis suggests an important role for cytokine antagonists in the regulation of HSC functions.

摘要

一个主要的限制因素,防止体内调节造血干细胞(HSCs)是不完全了解细胞和分子支持的微环境调节 HSC 命运的决定。因此,鼠 HSCs 不能被生成、维持或扩展在培养中延长一段时间。一个显著提高的理解骨髓龛环境及其与 HSCs 的分子相互作用是至关重要的,以克服这一挑战。我们在这里前瞻性地分离所有主要的非造血细胞龛成分,并详细地与龛细胞的标记或跟踪定义交叉相关。编译一个广泛的数据库的可溶性和膜结合配体 - 受体相互作用,我们开发了一种计算方法来推断潜在的细胞 - 细胞相互作用基于排序纯化的龛细胞和造血干细胞和祖细胞亚群的转录组数据。因此,我们建立了一个定义的龛组件和 HSCs 之间的分子通讯摘要。我们的分析表明细胞因子拮抗剂在调节 HSC 功能中的重要作用。

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