Literature DB >> 33384995

Limited Mitochondrial Activity Coupled With Strong Expression of CD34, CD90 and EPCR Determines the Functional Fitness of ex vivo Expanded Human Hematopoietic Stem Cells.

Luena Papa1, Mansour Djedaini1, Tiphaine C Martin2,3, Mahtab Zangui1, Kristin G Beaumont3, Robert Sebra3, Ramon Parsons2,3, Christoph Schaniel1,4,5, Ronald Hoffman1.   

Abstract

Ex vivo expansion strategies of human hematopoietic stem cell (HSC) grafts with suboptimal stem cell dose have emerged as promising strategies for improving outcomes of HSC transplantation in patients with hematological malignancies. While exposure of HSCs to ex vivo cultures expands the number of phenotypically identifiable HSCs, it frequently alters the transcriptomic and metabolic profiles, therefore, compromising their long-term (LT) hematopoietic reconstitution capacity. Within the heterogeneous pool of expanded HSCs, the precise phenotypic, transcriptomic and metabolic profile and thus, the identity of HSCs that confer LT repopulation potential remains poorly described. Utilizing valproic acid (VPA) in ex vivo cultures of umbilical cord blood (UCB)-CD34+ cells, we demonstrate that expanded HSCs phenotypically marked by expression of the stem cell markers CD34, CD90 and EPCR (CD201) are highly enriched for LT-HSCs. Furthermore, we report that low mitochondrial membrane potential, and, hence, mitochondrial activity distinguishes LT-HSCs within the expanded pool of phenotypically defined HSCs. Remarkably, such reduced mitochondrial activity is restricted to cells with the highest expression levels of CD34, CD90 and EPCR phenotypic markers. Together, our findings reveal that high expression of CD34, CD90 and EPCR in conjunction with low mitochondrial activity is critical for identification of functional LT-HSCs generated within ex vivo expansion cultures.
Copyright © 2020 Papa, Djedaini, Martin, Zangui, Beaumont, Sebra, Parsons, Schaniel and Hoffman.

Entities:  

Keywords:  CD90; EPCR; ex vivo expansion; functional fitness; mitochondrial membrane potential; phenotype; valproic acid

Year:  2020        PMID: 33384995      PMCID: PMC7769876          DOI: 10.3389/fcell.2020.592348

Source DB:  PubMed          Journal:  Front Cell Dev Biol        ISSN: 2296-634X


  65 in total

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Authors:  Eran Zimran; Luena Papa; Mansour Djedaini; Ami Patel; Camelia Iancu-Rubin; Ronald Hoffman
Journal:  Stem Cells Transl Med       Date:  2020-01-17       Impact factor: 6.940

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