3006 - 功能各异的巨核细胞祖细胞群在整个生命过程中以及在生理性和诱导性慢性炎症期间对造血的贡献各不相同

IF 2.5 4区 医学 Q2 HEMATOLOGY
Bryce Manso , Stephanie Smith-Berdan , Alessandra Rodriguez Y Baena , Lydia Mok , Paloma Medina , Marcel Rommel , Jenna Myers , Vanessa Jonsson , E. Camilla Forsberg
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引用次数: 0

摘要

随着年龄的增长,造血功能也会发生变化,包括造血干细胞(HSCs)和巨核细胞祖细胞(MkPs)的扩增,它们的表型和功能也会发生变化。MkPs的后代血小板也会发生与年龄相关的变化,从而引发炎症、心血管疾病和血栓性疾病,这些都是主要的健康问题。我们发现了一个非典型(ncMkP)群体,它在衰老过程中会发生特异性扩增。与典型的(cMkP)对应物相比,ncMkPs随着年龄的增长,扩张速度和存活率都有所提高。在移植和连续血液评估中,年轻和年老的 cMkPs 以及年轻的 ncMkPs 对血小板形成的贡献水平相似。相比之下,老年 ncMkPs 产生的血小板更多。随着年龄的增长,ncMkPs 的逐渐增加似乎部分源于造血干细胞,因为与年轻造血干细胞相比,老年造血干细胞体外生成 ncMkPs 的能力明显增强。此外,单细胞功能分析显示,这并不是由单个造血干细胞克隆驱动的,年轻和年老骨髓(BM)的单细胞 RNA 测序证实了这一发现。逐渐加重的慢性炎症被认为是衰老的一个驱动因素。在年轻小鼠中诱导慢性炎症可部分复制老年小鼠的已知特征,包括血小板输出量的改变和造血干细胞数量的增加,这表明慢性炎症在影响与年龄相关的血小板生成方面发挥着作用。通过体外培养对年轻和年老造血干细胞、cMkPs 和 ncMkPs 的炎症调节进行直接评估,发现了不同年龄和群体的特异性反应,揭示了直接炎症重编程令人惊讶的不同作用。这些新数据从机理上揭示了与衰老相关的不良血栓事件的细胞原因,并可能为缓解和恢复年轻化提供靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
3006 – FUNCTIONALLY DISTINCT MEGAKARYOCYTE PROGENITOR POPULATIONS DIFFERENTIALLY CONTRIBUTE TO HEMATOPOIESIS THROUGHOUT LIFE AND DURING PHYSIOLOGICAL AND INDUCED CHRONIC INFLAMMATION

Hematopoiesis changes upon aging, including expansion of hematopoietic stem cells (HSCs) and megakaryocyte progenitors (MkPs), which undergo changes in phenotype and function. Platelets, the progeny of MkPs, also undergo age-related alterations that drive inflammation and cardiovascular and thrombotic disease; major health concerns. We discovered a non-canonical (ncMkP) population that specifically expands upon aging. Compared to their canonical (cMkP) counterparts, ncMkPs exhibit increased expansion and survival with age. Upon transplantation and serial blood assessment, both young and old cMkPs, and young ncMkPs, contributed to similar levels of platelet formation. In contrast, aged ncMkPs specifically produced greater platelet output. The progressive increase in ncMkPs with age appears to be, in part, originating from HSCs as in vitro generation of ncMkPs was significantly enhanced by aged compared to young HSCs. Further, single-cell functional analysis revealed that this was not driven by individual HSC clones, a finding substantiated by single-cell RNA sequencing of young and old bone marrow (BM). Progressively increasing, chronic inflammation is thought to be a driver of aging. Inducing chronic inflammation in young mice partially phenocopies known features of aged mice, including altered platelet output and expanded HSC numbers, implicating its role in influencing age-related platelet production. Direct assessment of inflammatory modulation of young and old HSCs, cMkPs, and ncMkPs via in vitro culture revealed distinct age- and population-specific responses, uncovering surprisingly distinct and differential roles for direct inflammatory reprogramming. These new data provide mechanistic insight to cell-based causes of aging-related adverse thrombotic events and may offer targets for mitigation and rejuvenation.

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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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