| Literature DB >> 30971824 |
Anastasia N Tikhonova1,2, Igor Dolgalev3,4,5, Hai Hu3,4, Kishor K Sivaraj6, Edlira Hoxha3,4, Álvaro Cuesta-Domínguez7, Sandra Pinho8, Ilseyar Akhmetzyanova9, Jie Gao10, Matthew Witkowski3,4, Maria Guillamot3,4, Michael C Gutkin11, Yutong Zhang12, Christian Marier12, Catherine Diefenbach3,4, Stavroula Kousteni7, Adriana Heguy3,4,12, Hua Zhong13, David R Fooksman9, Jason M Butler11, Aris Economides10, Paul S Frenette8, Ralf H Adams6, Rahul Satija14, Aristotelis Tsirigos15,16,17, Iannis Aifantis18,19.
Abstract
The bone marrow microenvironment has a key role in regulating haematopoiesis, but its molecular complexity and response to stress are incompletely understood. Here we map the transcriptional landscape of mouse bone marrow vascular, perivascular and osteoblast cell populations at single-cell resolution, both at homeostasis and under conditions of stress-induced haematopoiesis. This analysis revealed previously unappreciated levels of cellular heterogeneity within the bone marrow niche and resolved cellular sources of pro-haematopoietic growth factors, chemokines and membrane-bound ligands. Our studies demonstrate a considerable transcriptional remodelling of niche elements under stress conditions, including an adipocytic skewing of perivascular cells. Among the stress-induced changes, we observed that vascular Notch delta-like ligands (encoded by Dll1 and Dll4) were downregulated. In the absence of vascular Dll4, haematopoietic stem cells prematurely induced a myeloid transcriptional program. These findings refine our understanding of the cellular architecture of the bone marrow niche, reveal a dynamic and heterogeneous molecular landscape that is highly sensitive to stress and illustrate the utility of single-cell transcriptomic data in evaluating the regulation of haematopoiesis by discrete niche populations.Entities:
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Year: 2019 PMID: 30971824 PMCID: PMC6607432 DOI: 10.1038/s41586-019-1104-8
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962