Transplanting rejuvenated blood stem cells extends lifespan of aged immunocompromised mice

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作者
Sara Montserrat-Vazquez
Noelle J. Ali
Francesca Matteini
Javier Lozano
Tu Zhaowei
Eva Mejia-Ramirez
Gina Marka
Angelika Vollmer
Karin Soller
Mehmet Sacma
Vadim Sakk
Loris Mularoni
Jan Philipp Mallm
Mireya Plass
Yi Zheng
Hartmut Geiger
M. Carolina Florian
机构
[1] L’Hospitalet de Llobregat,Stem Cell Aging Group, Regenerative Medicine Program, The Bellvitge Institute for Biomedical Research (IDIBELL)
[2] L’Hospitalet de Llobregat,Program for advancing the Clinical Translation of Regenerative Medicine of Catalonia, P
[3] University of Ulm,CMR[C]
[4] Cincinnati Children’s Hospital Medical Center,Institute of Molecular Medicine
[5] Biomaterials and Nanomedicine (CIBER-BBN),Division of Experimental Hematology and Cancer Biology
[6] DKFZ,Center for Networked Biomedical Research on Bioengineering
[7] L’Hospitalet de Llobregat,Gene Regulation of Cell Identity Group, Regenerative Medicine Program, The Bellvitge Institute for Biomedical Research (IDIBELL)
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摘要
One goal of regenerative medicine is to rejuvenate tissues and extend lifespan by restoring the function of endogenous aged stem cells. However, evidence that somatic stem cells can be targeted in vivo to extend lifespan is still lacking. Here, we demonstrate that after a short systemic treatment with a specific inhibitor of the small RhoGTPase Cdc42 (CASIN), transplanting aged hematopoietic stem cells (HSCs) from treated mice is sufficient to extend the healthspan and lifespan of aged immunocompromised mice without additional treatment. In detail, we show that systemic CASIN treatment improves strength and endurance of aged mice by increasing the myogenic regenerative potential of aged skeletal muscle stem cells. Further, we show that CASIN modifies niche localization and H4K16ac polarity of HSCs in vivo. Single-cell profiling reveals changes in HSC transcriptome, which underlie enhanced lymphoid and regenerative capacity in serial transplantation assays. Overall, we provide proof-of-concept evidence that a short systemic treatment to decrease Cdc42 activity improves the regenerative capacity of different endogenous aged stem cells in vivo, and that rejuvenated HSCs exert a broad systemic effect sufficient to extend murine health- and lifespan.
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