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In vitro and in vivo assessment of direct effects of simulated solar and galactic cosmic radiation on human hematopoietic stem/progenitor cells

机译:在体外和体内评估模拟太阳和银河宇宙射线对人类造血干/祖细胞的直接作用

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摘要

Future deep space missions to Mars and near-Earth asteroids will expose astronauts to chronic solar energetic particles (SEP) and galactic cosmic ray (GCR) radiation, and likely one or more solar particle events (SPEs). Given the inherent radiosensitivity of hematopoietic cells and short latency period of leukemias, space radiation-induced hematopoietic damage poses a particular threat to astronauts on extended missions. We show that exposing human hematopoietic stem/progenitor cells (HSC) to extended mission-relevant doses of accelerated high-energy protons and iron ions leads to the following: (1) introduces mutations that are frequently located within genes involved in hematopoiesis and are distinct from those induced by γ-radiation; (2) markedly reduces in vitro colony formation; (3) markedly alters engraftment and lineage commitment in vivo; and (4) leads to the development, in vivo, of what appears to be T-ALL. Sequential exposure to protons and iron ions (as typically occurs in deep space) proved far more deleterious to HSC genome integrity and function than either particle species alone. Our results represent a critical step for more accurately estimating risks to the human hematopoietic system from space radiation, identifying and better defining molecular mechanisms by which space radiation impairs hematopoiesis and induces leukemogenesis, as well as for developing appropriately targeted countermeasures.
机译:未来对火星和近地小行星的深空飞行任务会将宇航员暴露于长期的太阳高能粒子(SEP)和银河宇宙射线(GCR)辐射下,并可能使其遭受一次或多次太阳粒子事件(SPEs)。考虑到造血细胞固有的放射敏感性和白血病的潜伏期短,空间辐射引起的造血功能损害对航天员在执行长期任务时具有特别的威胁。我们显示,将人类造血干/祖细胞(HSC)暴露于与任务相关的扩展剂量的加速高能质子和铁离子,会导致以下情况:(1)引入经常位于参与造血的基因内的突变由γ射线诱导的那些; (2)明显减少体外菌落的形成; (3)显着改变体内的植入和血统承诺; (4)导致体内似乎是T-ALL的发展。连续暴露于质子和铁离子(通常发生在深空)对HSC基因组完整性和功能的危害远远大于单独的任何一种颗粒。我们的结果代表了至关重要的一步,它是更准确地估计太空辐射对人类造血系统的风险,识别和更好地定义太空辐射损害造血作用并诱导白血病发生的分子机制,以及制定适当针对性对策的关键步骤。

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