A comprehensive transcriptome signature of murine hematopoietic stem cell aging

Author:

Flohr Svendsen Arthur1ORCID,Yang Daozheng1,Kim KyungMok2,Lazare Seka1ORCID,Skinder Natalia1,Zwart Erik1ORCID,Mura-Meszaros Anna2,Ausema Albertina1,von Eyss Björn2ORCID,de Haan Gerald1ORCID,Bystrykh Leonid1ORCID

Affiliation:

1. European Research Institute for the Biology of Ageing, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands; and

2. Transcriptional Control of Tissue Homeostasis Laboratory, Leibniz Institute on Aging, Fritz Lipmann Institute e.V., Jena, Germany

Abstract

Abstract We surveyed 16 published and unpublished data sets to determine whether a consistent pattern of transcriptional deregulation in aging murine hematopoietic stem cells (HSC) exists. Despite substantial heterogeneity between individual studies, we uncovered a core and robust HSC aging signature. We detected increased transcriptional activation in aged HSCs, further confirmed by chromatin accessibility analysis. Unexpectedly, using 2 independent computational approaches, we established that deregulated aging genes consist largely of membrane-associated transcripts, including many cell surface molecules previously not associated with HSC biology. We show that Selp (P-selectin), the most consistent deregulated gene, is not merely a marker for aged HSCs but is associated with HSC functional decline. Additionally, single-cell transcriptomics analysis revealed increased heterogeneity of the aged HSC pool. We identify the presence of transcriptionally “young-like” HSCs in aged bone marrow. We share our results as an online resource and demonstrate its utility by confirming that exposure to sympathomimetics or deletion of Dnmt3a/b molecularly resembles HSC rejuvenation or aging, respectively.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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