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供者造血干细胞通过自我更新分裂超过宿主细胞,从而长期重建骨髓。

Donor hematopoietic stem cells confer long-term marrow reconstitution by self-renewal divisions exceeding to that of host cells.

机构信息

Stem Cell Biology, National Institute of Immunology, New Delhi, India.

出版信息

PLoS One. 2012;7(12):e50693. doi: 10.1371/journal.pone.0050693. Epub 2012 Dec 5.

Abstract

Dormant hematopoietic stem cells (HSCs) are activated by microenvironmental cues of the niche in response to the injury of bone marrow (BM). It is not clearly understood how engrafted cells respond to these cues and are involved in marrow regeneration. The purpose of this study was to decipher this cellular response in competitive environment. BM cells of CD45.2 mice were transplanted in sub-lethally irradiated CD45.1 mice. The status of the donor and recipient stem cells (LSK: Lin(-)Sca-1(+)c-Kit(+)) were determined by flowcytometry using CD45 alleles specific antibodies. The presence of long-term engraftable stem cells was confirmed by marrow repopulation assay in secondary hosts, and cell cycle status was determined by staining with Ho33342 and pyronin Y, and BrdU retention assay. The expressions of different hematopoietic growth factor genes in stromal compartment (CD45(-) cells) were assessed by real-time reverse transcriptase- polymerase chain reaction (RT-PCR). The presence of donor cells initially stimulated the proliferation of host LSK cells compared with control mice without transplantation. This was expected due to pro-mitotic and anti-apoptotic factors secreted by the donor hematopoietic cells. Upon transplantation, a majority of the donor LSK cells entered into cell cycle, and later they maintained cell cycle status similar to that in the normal mouse. Donor-derived LSK cells showed 1000-fold expansion within 15 days of transplantation. Donor-derived cells not only regenerated BM in the primary irradiated host for long-term, they were also found to be significantly involved in marrow regeneration after the second cycle of irradiation. The proliferation of LSK cells was associated with the onset of colossal expression of different hematopoietic growth factor genes in non-hematopoietic cellular compartment. Activation of donor LSK cells was found to be dynamically controlled by BM cellularity. Long-term study showed that a high level of hematopoietic reconstitution could be possible by donor cells in a sub-lethally irradiated host.

摘要

休眠造血干细胞(HSCs)在骨髓损伤时,通过龛的微环境线索被激活。目前尚不清楚植入细胞如何响应这些线索并参与骨髓再生。本研究旨在解析这种细胞反应在竞争环境下的过程。通过流式细胞术使用 CD45 等位基因特异性抗体,检测 CD45.2 小鼠的 BM 细胞在亚致死照射的 CD45.1 小鼠中的状态。通过在二级宿主中的骨髓再植入实验来确认长期可植入干细胞的存在,并通过 Ho33342 和吡罗红 Y 染色以及 BrdU 保留实验来确定细胞周期状态。通过实时逆转录-聚合酶链反应(RT-PCR)评估基质细胞(CD45(-)细胞)中不同造血生长因子基因的表达。与未移植的对照小鼠相比,供体细胞的存在最初刺激了宿主 LSK 细胞的增殖。这是由于供体造血细胞分泌的促有丝分裂和抗凋亡因子所致。移植后,大多数供体 LSK 细胞进入细胞周期,随后它们维持与正常小鼠相似的细胞周期状态。移植后 15 天内,供体 LSK 细胞扩增了 1000 倍。供体来源的细胞不仅在原照射宿主中长期再生 BM,而且在第二次照射循环后也被发现显著参与骨髓再生。LSK 细胞的增殖与不同造血生长因子基因在非造血细胞区室中巨量表达的开始相关。供体 LSK 细胞的激活被发现受到 BM 细胞数量的动态控制。长期研究表明,在亚致死照射的宿主中,供体细胞可以实现高水平的造血重建。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/642a/3515605/c2e105f30e77/pone.0050693.g001.jpg

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