Engineering a haematopoietic stem cell niche by revitalizing mesenchymal stromal cells

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作者
Fumio Nakahara
Daniel K. Borger
Qiaozhi Wei
Sandra Pinho
Maria Maryanovich
Ali H. Zahalka
Masako Suzuki
Cristian D. Cruz
Zichen Wang
Chunliang Xu
Philip E. Boulais
Avi Ma’ayan
John M. Greally
Paul S. Frenette
机构
[1] Ruth L. and David S. Gottesman Institute for Stem Cell and Regenerative Medicine Research,Department of Cell Biology
[2] Albert Einstein College of Medicine,Department of Medicine
[3] Albert Einstein College of Medicine,Center for Epigenomics, Department of Genetics
[4] Albert Einstein College of Medicine,Department of Pharmacological Sciences, Mount Sinai Center for Bioinformatics
[5] Albert Einstein College of Medicine,Department of Hematology and Oncology, Graduate School of Medicine
[6] Icahn School of Medicine at Mount Sinai,undefined
[7] The University of Tokyo,undefined
来源
Nature Cell Biology | 2019年 / 21卷
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摘要
Haematopoietic stem cells (HSCs) are maintained by bone marrow niches in vivo1,2, but the ability of niche cells to maintain HSCs ex vivo is markedly diminished. Expression of niche factors by Nestin-GFP+ mesenchymal-derived stromal cells (MSCs) is downregulated upon culture, suggesting that transcriptional rewiring may contribute to this reduced HSC maintenance potential. Using an RNA sequencing screen, we identified five genes encoding transcription factors (Klf7, Ostf1, Xbp1, Irf3 and Irf7) that restored HSC niche function in cultured bone marrow-derived MSCs. These revitalized MSCs (rMSCs) exhibited enhanced synthesis of HSC niche factors while retaining their mesenchymal differentiation capacity. In contrast to HSCs co-cultured with control MSCs, HSCs expanded with rMSCs showed higher repopulation capacity and protected lethally irradiated recipient mice. Competitive reconstitution assays revealed an approximately sevenfold expansion of functional HSCs by rMSCs. rMSCs prevented the accumulation of DNA damage in cultured HSCs, a hallmark of ageing and replication stress. Analysis of the reprogramming mechanisms uncovered a role for myocyte enhancer factor 2c (Mef2c) in the revitalization of MSCs. These results provide insight into the transcriptional regulation of the niche with implications for stem cell-based therapies.
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页码:560 / 567
页数:7
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