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Large-Scale Clonal Analysis Resolves Aging of the Mouse Hematopoietic Stem Cell Compartment

机译:大规模克隆分析解决了小鼠造血干细胞舱的老化

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摘要

Aging is linked to functional deterioration and hematological diseases. The hematopoietic system is maintained by hematopoietic stem cells (HSCs), and dysfunction within the HSC compartment is thought to be a key mechanism underlying age-related hematopoietic perturbations. Using single-cell transplantation assays with five blood-lineage analysis, we previously identified myeloid-restricted repopulating progenitors (MyRPs) within the phenotypic HSC compartment in young mice. Here, we determined the age-related functional changes to the HSC compartment using over 400 single-cell transplantation assays. Notably, MyRP frequency increased dramatically with age, while multipotent HSCs expanded modestly within the bone marrow. We also identified a subset of functional cells that were myeloid restricted in primary recipients but displayed multipotent (five blood-lineage) output in secondary recipients. We have termed this cell type?latent-HSCs, which appear exclusive to the aged HSC compartment. These results question the traditional dogma of HSC aging and our current approaches to assay and define HSCs.
机译:老化与功能性劣化和血液疾病有关。造血系统由造血干细胞(HSC)保持,HSC隔室内的功能障碍被认为是相关年龄相关造血扰动的关键机制。使用具有五种血液谱分析的单细胞移植测定,我们先前鉴定了年轻小鼠的表型HSC隔间内的髓样限制较重新血压祖细胞(MYRP)。在这里,我们使用400个单细胞移植测定确定与HSC隔间相关的年龄相关的功能变化。值得注意的是,MYRP频率随着年龄的增长而显着增加,而多能HSC在骨髓内膨胀。我们还确定了在初级接受者中限制的肌电细胞的功能细胞的子集,但在辅助收件人中显示了多能(五种血统)输出。我们称之为这种细胞类型?潜在的HSC,它看起来是老年的HSC盒子。这些结果质疑HSC老化的传统教条和我们目前的测定方法和定义HSC。

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