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衰老对灵长类动物造血作用的影响可通过克隆追踪来研究。

The impact of aging on primate hematopoiesis as interrogated by clonal tracking.

机构信息

Hematology Branch, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD.

Department of Microbiology and Immunology, Georgetown University Medical Center, Washington, DC.

出版信息

Blood. 2018 Mar 15;131(11):1195-1205. doi: 10.1182/blood-2017-08-802033. Epub 2018 Jan 2.

Abstract

Age-associated changes in hematopoietic stem and progenitor cells (HSPCs) have been carefully documented in mouse models but poorly characterized in primates and humans. To investigate clinically relevant aspects of hematopoietic aging, we compared the clonal output of thousands of genetically barcoded HSPCs in aged vs young macaques after autologous transplantation. Aged macaques showed delayed emergence of output from multipotent (MP) clones, with persistence of lineage-biased clones for many months after engraftment. In contrast to murine aging models reporting persistence of myeloid-biased HSPCs, aged macaques demonstrated persistent output from both B-cell and myeloid-biased clones. Clonal expansions of MP, myeloid-biased, and B-biased clones occurred in aged macaques, providing a potential model for human clonal hematopoiesis of indeterminate prognosis. These results suggest that long-term MP HSPC output is impaired in aged macaques, resulting in differences in the kinetics and lineage reconstitution patterns between young and aged primates in an autologous transplantation setting.

摘要

年龄相关的造血干细胞和祖细胞(HSPCs)变化在小鼠模型中已被详细记录,但在灵长类动物和人类中特征描述较差。为了研究与造血衰老相关的临床方面,我们比较了年老和年轻恒河猴自体移植后数千个遗传标记的 HSPC 克隆的克隆输出。年老的恒河猴显示出多能(MP)克隆输出出现延迟,在植入后数月内仍然存在谱系偏向的克隆。与报告髓系偏向 HSPC 持续存在的小鼠衰老模型相反,年老的恒河猴表现出 B 细胞和髓系偏向克隆的持续输出。MP、髓系偏向和 B 细胞偏向克隆的克隆扩增发生在年老的恒河猴中,为具有不确定预后的人类克隆性造血提供了一个潜在的模型。这些结果表明,年老的恒河猴中长期 MP HSPC 输出受损,导致在自体移植环境中年轻和年老灵长类动物之间的动力学和谱系重建模式存在差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/770b/5855019/b5284f26e03d/blood802033absf1.jpg

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