| Literature DB >> 29295845 |
Kyung-Rok Yu1, Diego A Espinoza1, Chuanfeng Wu1, Lauren Truitt1, Tae-Hoon Shin1, Shirley Chen1, Xing Fan1, Idalia M Yabe1,2, Sandhya Panch1, So Gun Hong1, Samson Koelle1,3, Rong Lu4, Aylin Bonifacino1, Allen Krouse1, Mark Metzger1, Robert E Donahue1, Cynthia E Dunbar1.
Abstract
Age-associated changes in hematopoietic stem and progenitor cells (HSPCs) have been carefully documented in mouse models but poorly characterized in primates and humans. To investigate clinically relevant aspects of hematopoietic aging, we compared the clonal output of thousands of genetically barcoded HSPCs in aged vs young macaques after autologous transplantation. Aged macaques showed delayed emergence of output from multipotent (MP) clones, with persistence of lineage-biased clones for many months after engraftment. In contrast to murine aging models reporting persistence of myeloid-biased HSPCs, aged macaques demonstrated persistent output from both B-cell and myeloid-biased clones. Clonal expansions of MP, myeloid-biased, and B-biased clones occurred in aged macaques, providing a potential model for human clonal hematopoiesis of indeterminate prognosis. These results suggest that long-term MP HSPC output is impaired in aged macaques, resulting in differences in the kinetics and lineage reconstitution patterns between young and aged primates in an autologous transplantation setting.Entities:
Mesh:
Year: 2018 PMID: 29295845 PMCID: PMC5855019 DOI: 10.1182/blood-2017-08-802033
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113