2022 - 老年造血:超越造血干细胞功能障碍的决定论教条

IF 2.5 4区 医学 Q2 HEMATOLOGY
Charles Dussiau , Foteini Fotopoulou , Esther Rodriguez-Correa , Ian Ghezzi , Melanie Ball , Franziska Pilz , Jeyan Jayarajan , Susanne Lux , Theo Aurich , Ruzhica Bogeska , Sood Shubhankar , Marieke Essers , Judith Zaugg , Michael Milsom
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引用次数: 0

摘要

机体衰老被认为是由多种遗传和环境变量长期累积作用的相互作用所介导的,这混淆了对这一过程的机理认识。在这项研究中,我们测量了在同一受控环境中饲养的一大批(100 只)幼年(8 周)、中年(18 个月)和老年(24 个月)雌性 C57BL/6J 小鼠造血组织的各种血液学变量(细胞计数、组织学、流式细胞术、造血干细胞移植、scRNA 和 scATAC-seq)。令人惊讶的是,尽管基因型和环境的差异极小,但整个群体的老年表型差异很大,一些 24 个月大的小鼠表现出与 8 周大对照组一致的参数,而另一些则表现出极端的老年结果。这表明造血衰老有一个主要的随机基础,而文献中很少考虑到这一点。重要的是,被认为具有因果关系的典型年龄相关表型(造血干细胞功能潜能、造血干细胞扩增、骨髓偏倚、贫血)在整个群体中的相关性很差,这对造血干细胞功能障碍驱动老年造血进化的观点提出了挑战。对骨髓造血干细胞、祖细胞、成熟造血细胞和生态位细胞进行 scRNA 序列分析,发现了一个新的炎性脂肪前体细胞群体,该群体为老年个体所独有,但在老年个体中具有异质性。相互作用分析表明,这些细胞接收来自中性粒细胞的炎症信号(Il1b 和 Tnf),并下调通常向造血干细胞发出信号的配体(Kitl、Vcam1 和 Angpt2),从而有可能在衰老过程中介导造血干细胞的衰退。综上所述,这些发现对造血干细胞受损导致的统一血液学衰老过程的观点提出了质疑,而是表明这是一个随机过程,并延伸到异质性的生态位组成。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
2022 – AGING HEMATOPOIESIS: BEYOND THE DETERMINISTIC DOGMA OF HEMATOPOIETIC STEM CELL DYSFUNCTION

Organismal aging is thought to be mediated by the interaction of multiple genetic and environmental variables acting cumulatively over long periods of time, confounding mechanistic insights into this process. In this study, we measured a wide range of hematologic variables (cell counts, histology, flow cytometry, HSC transplantation, scRNA and scATAC-seq) from hematopoietic tissues across a large cohort (>100 individuals) of young (8 weeks), middle aged (18 months) and old (>24 months) female C57BL/6J mice housed in the same controlled environment. Surprisingly, the aged phenotypes across the cohort were highly variable, with some 24-month-old mice displaying parameters in line with 8-week-old controls while others demonstrating extreme aged outcomes, despite the minimal variance in genotype and environment. This suggests a dominant stochastic basis to hematopoietic aging that is rarely considered in the literature. Importantly, canonical age-associated phenotypes that are thought to have a causal relationship (HSC functional potential, HSC expansion, myeloid bias, anemia) poorly correlated across the cohort, challenging the concept that HSC dysfunction drives the evolution of aged hematopoiesis. scRNAseq of bone marrow HSCs, progenitors, mature hematopoietic and niche cells identified a new population of inflammatory adipocytes precursors exclusive to, but heterogenous across aged individuals. Interaction analysis suggests that these cells receive inflammatory signals from neutrophils (Il1b and Tnf), and downregulate ligands (Kitl, Vcam1, and Angpt2) that typically signal to HSCs, potentially mediating HSC decline during aging. Taken together, these findings challenge the notion of a uniform hematological aging process stemming from compromised HSCs, but rather indicate a stochastic process, which extends to a heterogenous niche composition.

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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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