2010 – THE PROTEOSTASIS NETWORK IS DYNAMICALLY REGULATED THROUGHOUT HEMATOPOIETIC STEM CELL ONTOGENY

IF 2.5 4区 医学 Q2 HEMATOLOGY Experimental hematology Pub Date : 2024-08-01 DOI:10.1016/j.exphem.2024.104567
Helena Yu , Robert Signer
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引用次数: 0

Abstract

Hematopoietic stem cells (HSCs) establish hematopoiesis and maintain regeneration of blood and immune cells to meet shifting demands for blood cell production during development and throughout life. The protein homeostasis (proteostasis) network is uniquely configured in adult HSCs to preserve stem cell fitness and longevity. However, how proteostasis is regulated in developing HSCs is largely unexplored. Here, we comprehensively analyzed proteostasis network activity throughout fetal and neonatal development. Fetal HSCs exhibited up to 7-fold higher protein synthesis rates than their adult counterparts but contained similarly low amounts of unfolded and misfolded proteins as adult HSCs without substantial shifts in protein degradation activity. These data suggested that fetal and adult HSCs utilize distinct mechanisms to preserve proteostasis. We found that fetal HSCs preferentially activated Hsf1, a key proteostasis sensor, and preferentially expressed multiple Hsf1 target genes. Deletion of Hsf1 in the developing hematopoietic system altered HSC ontogeny during the transition from the fetal liver to the bone marrow. Strikingly, HSCs exhibited a dramatic spike in unfolded protein abundance at birth, raising the question of whether proteostasis disruption impairs the function of temporally analogous human umbilical cord blood-derived HSCs. To test this, cord blood CD34+ cells were sorted based on unfolded protein content. Cord blood hematopoietic stem and progenitor cells with low unfolded protein content formed up to 9-fold more colonies than cells with high unfolded protein, which also exhibited diminished reconstituting activity in vivo. Overall, distinct regulation of proteostasis is a key developmental feature of HSCs that could be leveraged to optimize HSC-based therapeutics.

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2010 - 蛋白稳态网络在造血干细胞的整个发育过程中受到动态调控
造血干细胞(HSCs)建立造血功能,维持血液和免疫细胞的再生,以满足发育过程中和整个生命过程中对血细胞生成不断变化的需求。成年造血干细胞中的蛋白质平衡(蛋白稳态)网络配置独特,可保持干细胞的健康和寿命。然而,发育中的造血干细胞如何调节蛋白稳态在很大程度上尚未被探索。在这里,我们全面分析了整个胎儿和新生儿发育过程中蛋白稳态网络的活动。胎儿造血干细胞的蛋白质合成率是成人造血干细胞的7倍,但其含有的未折叠和折叠错误蛋白质的数量与成人造血干细胞相似,蛋白质降解活性没有发生实质性变化。这些数据表明,胎儿造血干细胞和成体造血干细胞利用不同的机制来维持蛋白稳态。我们发现,胎儿造血干细胞优先激活关键蛋白稳态传感器 Hsf1,并优先表达多个 Hsf1 靶基因。在发育中的造血系统中缺失Hsf1会改变造血干细胞从胎儿肝脏向骨髓过渡的本体发生。令人震惊的是,造血干细胞在出生时表现出未折叠蛋白丰度的急剧飙升,这就提出了一个问题:蛋白稳态的破坏是否会损害时间上类似的人类脐带血造血干细胞的功能?为了验证这一点,我们根据未折叠蛋白的含量对脐带血CD34+细胞进行了分拣。未折叠蛋白含量低的脐带血造血干细胞和祖细胞形成的集落数量是未折叠蛋白含量高的细胞的9倍,而未折叠蛋白含量高的细胞在体内的重组活性也较弱。总之,对蛋白稳态的独特调节是造血干细胞的一个关键发育特征,可用于优化以造血干细胞为基础的疗法。
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来源期刊
Experimental hematology
Experimental hematology 医学-血液学
CiteScore
5.30
自引率
0.00%
发文量
84
审稿时长
58 days
期刊介绍: Experimental Hematology publishes new findings, methodologies, reviews and perspectives in all areas of hematology and immune cell formation on a monthly basis that may include Special Issues on particular topics of current interest. The overall goal is to report new insights into how normal blood cells are produced, how their production is normally regulated, mechanisms that contribute to hematological diseases and new approaches to their treatment. Specific topics may include relevant developmental and aging processes, stem cell biology, analyses of intrinsic and extrinsic regulatory mechanisms, in vitro behavior of primary cells, clonal tracking, molecular and omics analyses, metabolism, epigenetics, bioengineering approaches, studies in model organisms, novel clinical observations, transplantation biology and new therapeutic avenues.
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