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Functional Niche Competition Between Normal Hematopoietic Stem and Progenitor Cells and Myeloid Leukemia Cells

机译:正常造血干细胞和祖细胞与髓样白血病细胞之间的功能性利基竞争

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摘要

Hematopoietic stem and progenitor cells (HSPC) reside in a specialized niche that regulates their proliferative capacity and their fate. There is increasing evidence for similar roles of marrow niches on controlling the behavior of leukemic cells, however whether normal HSC and leukemic cells reside in or functionally compete for the same marrow niche is unclear. We used the MLL-AF9 murine acute myeloid leukemia in a competitive repopulation model to investigate whether normal HSPC and leukemic cells functionally compete for the same marrow niches. Irradiated recipient mice were transplanted with fixed numbers of MLL-AF9 cells mixed with increasing doses of normal syngeneic whole bone marrow (WBM) or with purified HSPC (LSK). Survival was significantly increased and leukemic progression was delayed proportional to increasing doses of normal WBM or normal LSK cells in multiple independent experiments, with all doses of WBM or LSK cells studied above the threshold for rapid and complete hematopoietic reconstitution in the absence of leukemia. Confocal microscopy demonstrated nests of either leukemic cells or normal hematopoietic cells but not both in the marrow adjacent to endosteum. Early following transplantation, leukemic cells from animals receiving lower LSK doses were cycling more actively than in those receiving higher doses. These results suggest that normal HSPC and AML cells compete for the same functional niche. Manipulation of the niche could impact on response to anti-leukemic therapies, and the numbers of normal HSPC could impact on leukemia outcome, informing approaches to cell dose in the context of stem cell transplantation.
机译:造血干细胞和祖细胞(HSPC)位于一个专门的小生境中,可以调节其增殖能力和命运。越来越多的证据表明,骨髓小生境在控制白血病细胞的行为中具有相似的作用,但是尚不清楚正常的HSC和白血病细胞是否位于相同的骨髓生境中或在功能上竞争相同的骨髓生境。我们在竞争性种群模型中使用了MLL-AF9小鼠急性髓性白血病,以调查正常的HSPC和白血病细胞是否在功能上竞争相同的骨髓小生境。用固定数量的MLL-AF9细胞与增加剂量的正常同基因全骨髓(WBM)或纯化的HSPC(LSK)混合,对接受辐照的小鼠进行移植。在多个独立实验中,存活率显着增加,并且白血病进展与正常WBM或正常LSK细胞剂量的增加成比例地延迟,在没有白血病的情况下,所有剂量的WBM或LSK细胞的研究都超过了快速,完全造血重建的阈值。共聚焦显微镜检查显示白血病细胞或正常造血细胞的巢,但并非两者都在邻近内膜的骨髓中。移植后的早期,来自接受较低LSK剂量的动物的白血病细胞比接受较高剂量的动物的白血病细胞更活跃地循环。这些结果表明正常的HSPC和AML细胞竞争相同的功能位。适当位置的操纵可能会影响对抗白血病疗法的反应,而正常HSPC的数量可能会影响白血病的结果,从而在干细胞移植的背景下为细胞剂量的研究提供依据。

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