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Establishment of neutrophil-lineage stem cells from C57BL/6 mice

机译:C57BL / 6小鼠中性粒细胞谱系干细胞的建立

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Neutrophils are key effector player of the innate immune system that are rapidly recruited to infected tissues to clear pathogens. Neutrophils also have the capacity to engulf damaged tissue cells to clear, although at the same time neutrophil granules including myeloperioxidase, elastase and ROS may damage tissues. We have shown previously that neutrophils help to repair wounded tissue. However, neutrophils are already differentiated cells, which cannot divide. For future personalized stem cells therapy, it is important to establish neutrophil-precursor cells, which will differentiate to mature neutrophils to engulf pathogens or damaged cells by the transplantation in vivo. First we characterized 32Dcl3 cell line, which has been established previously by WEHI-3 conditional medium. These cell lines differentiated to neutrophils by the stimulation of G-CSF. Then we established similar clone from C57BL/6 mice by culturing bone marrow cells in WEHI-3 conditional medium. We could obtain a neutrophil-precursor cell line (B6NPC), which grows more than six months in WEHI-3 conditional medium. By FACS analysis, we found that both 32Dcl3 and B6NPC had GR-1, CD11b and F4/80 cell surface markers, which are myeloid-lineage markers. However, these cells also have early T cell markers, which fit the hypothesis of myeloid-based model of hematopoietic cell differentiation. By the transplantation of B6NPC to syngeneic mice at the same time of wounding, we found early recovery from wound healing.
机译:中性粒细胞是先天免疫系统的关键效应因子,其被迅速募集到感染的组织中以清除病原体。中性粒细胞还具有吞噬受损组织细胞的能力,尽管同时包括髓过氧化物酶,弹性蛋白酶和ROS的中性粒细胞颗粒可能会破坏组织。先前我们已经证明中性粒细胞有助于修复受伤的组织。但是,中性粒细胞已经是分化的细胞,不能分裂。对于将来的个性化干细胞疗法,重要的是建立中性粒细胞前体细胞,该细胞将通过体内移植分化为成熟的中性粒细胞,以吞噬病原体或受损的细胞。首先,我们表征了32Dcl3细胞系,该细胞系先前已由WEHI-3条件培养基建立。这些细胞系通过刺激G-CSF分化为嗜中性粒细胞。然后,我们通过在WEHI-3条件培养基中培养骨髓细胞,从C57BL / 6小鼠中建立了相似的克隆。我们可以获得中性粒细胞前体细胞系(B6NPC),它在WEHI-3条件培养基中生长超过六个月。通过FACS分析,我们发现32Dcl3和B6NPC都具有GR-1,​​CD11b和F4 / 80细胞表面标记,它们是髓系谱系标记。但是,这些细胞也具有早期的T细胞标记,这符合基于骨髓的造血细胞分化模型的假设。通过在受伤的同时将B6NPC移植到同系小鼠中,我们发现伤口愈合可以尽早恢复。

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