Adult human megakaryocyte-erythroid progenitors are in the CD34+CD38mid fraction

Sanada, Chad; Xavier-Ferrucio, Juliana; Lu, Yi-Chien; Min, Elizabeth; Zhang, Ping-Xia; Zou, Siying; Yong, Kang; Zhang, Meng; Zerafati, Gazelle; Gallagher, Patrick G.; Krause, Diane S.

doi:10.1182/blood-2016-01-693705

Cited by 55 publications

(77 citation statements)

References 40 publications

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“…While our work still supports a model for progressive restriction of developmental potential, it suggests that these events are clonally heterogeneous and occur much earlier in the hematopoietic hierarchy, in line with recent data 7,8,14,16 . Though our data fail to provide any evidence for CMP or MEP fates in situ , many experiments have provided evidence for MEP-like cells at a clonal level 4,12,13,24 . We posit that while Mk-Er bipotential exists in transplant or culture setting, this fate is not substantially manifested in unperturbed conditions.…”

contrasting

confidence: 93%

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Clonal analysis of lineage fate in native haematopoiesis

Rodriguez-Fraticelli

Wolock

Weinreb

et al. 2018

Nature

430

413

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SUMMARY Hematopoiesis, the process of mature blood and immune cell production, is functionally organized as a hierarchy, with self-renewing hematopoietic stem cells (HSCs) and multipotent progenitor (MPP) cells sitting at the very top1,2. Multiple models have been proposed as to what the earliest lineage choices are in these primitive hematopoietic compartments, the cellular intermediates, and the resulting lineage trees that emerge from them3–10. Given that the bulk of studies addressing lineage outcomes have been performed in the context of hematopoietic transplantation, current lineage branching models are more likely to represent roadmaps of lineage potential rather than native fate. Here, we utilize transposon (Tn) tagging to clonally trace the fates of progenitors and stem cells in unperturbed hematopoiesis. Our results describe a distinct clonal roadmap in which the megakaryocyte (Mk) lineage arises largely independently of other hematopoietic fates. Our data, combined with single cell RNAseq, identify a functional hierarchy of uni- and oligolineage producing clones within the MPP population. Finally, our results demonstrate that traditionally defined long-term HSCs (LT-HSCs) are a significant source of Mk-restricted progenitors, suggesting that the Mk-lineage is the predominant native fate of LT-HSCs. Our study provides evidence for a substantially revised roadmap for unperturbed hematopoiesis, and highlights unique properties of MPPs and HSCs in situ.

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confidence: 93%

“…1d–e and Extended Data Fig. 4b) 12,13 . At 8 weeks, our analysis revealed the activity of a set of multilineage clones (239±58), with lymphoid (B), My and Er contribution, but still with no presence in Mk, indicating the existence of Mk-deficient lympho-erythromyeloid (LEM) progenitors (Fig.…”

mentioning

confidence: 91%

Clonal analysis of lineage fate in native haematopoiesis

Rodriguez-Fraticelli

Wolock

Weinreb

et al. 2018

Nature

430

413

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“…While not widely appreciated, all hematopoietic stem cells and most hematopoietic progenitor cells (including multi potent progenitor (MPP) and common myeloid progenitor (CMP), but excluding committed erythroid progenitors) express MPL, the receptor for TPO, on their cell membranes. [5, 10–13]…”

Section: Megakaryopoiesis and Erythropoiesismentioning

confidence: 99%

“…However, early experiments by Debili et al found dual-lineage (Mk and erythroid) colonies composed of 100 to 1,000 erythroblasts intermixed with a few MK that were enriched in the CD34+CD38+/− and CD34+CD38− cell fractions. Even though CD34+CD38high human cells have been published as being greatly enriched for erythroid committed cells,[10] papers still use this gate to isolate what they refer to as human “MEP.” Consequently, single cell RNA sequencing data from this population shows that many of these cells are erythroid committed, which would lead investigators to question the existence of human MEPs. [27, 28]…”

Section: Challenges In Isolating Mepmentioning

confidence: 99%

Concise Review: Bipotent Megakaryocytic-Erythroid Progenitors: Concepts and Controversies

Xavier-Ferrucio

Krause

2018

Stem Cells

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Hematopoietic stem and progenitor cells maintain blood formation throughout our lifetime by undergoing long- and short-term self-renewal, respectively. As progenitor cells progress through the hematopoiesis process, their differentiation capabilities narrow, such that the precursors become committed to only one or two lineages. This Review focuses on recent advances in the identification and characterization of bipotent megakaryocytic-erythroid progenitors (MEP), the cells that can further produce two completely different functional outputs: platelets and red blood cells. The existence of MEP has sparked controversy as studies describing the requirement for this intermediate progenitor stage prior to commitment to the erythroid and megakaryocytic lineages have been potentially contradictory. Interpretation of these studies is complicated by the variety of species, cell sources, and analytical approaches used along with inherent challenges in the continuum of hematopoiesis, where hematopoietic progenitors do not stop at discrete steps on single paths as classically drawn in hematopoietic hierarchy models. With the goal of improving our understanding of human hematopoiesis, we discuss findings in both human and murine cells. Based on these data, MEP clearly represent a transitional stage of differentiation in at least one route to the generation of both megakaryocytes and erythroid cells. Stem Cells 2018;36:1138-1145.

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“…As summarized in Table 1, MEPs have been characterized using a combination of cell surface markers including IL-3R, FLT3, MPL (assessed using BAH1 clone and other antibodies), CD36, CD41, CD71 and CD105 (8*, 9*, 10**, 14**). Using a combination of approaches including functional, single cell transcriptomics and lineage potential assays, these studies reveal that the identification of MEP and their subpopulations appears highly dependent on gating strategy; this likely reflects their extensive heterogeneity.…”

Section: Isolation and Characterization Of Megakaryocyte-erythroid Anmentioning

confidence: 99%

Characterization, regulation, and targeting of erythroid progenitors in normal and disordered human erythropoiesis

Dulmovits

Hom

Narla

et al. 2017

Current Opinion in Hematology

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Purpose of review The erythroid progenitors BFU-E (burst-forming unit-erythroid) and CFU-E (colony-forming unit-erythroid) have a critical role in erythropoiesis. They represent a heterogeneous and poorly characterized population of cells with modifiable self-renewal, proliferation and differentiation capabilities. This review focuses on the current state of erythroid progenitor biology with regard to immunophenotypic identification and regulatory programs; in addition, we will discuss the therapeutic implications of using these erythroid progenitors as pharmacologic targets. Recent findings Erythroid progenitors are classically defined by the appearance of morphologically defined colonies in semisolid cultures. However, these prior systems preclude a more thorough understanding of the composite nature of progenitor populations. Recent studies employing novel flow cytometric and cell-based assays have helped to redefine hematopoiesis, and suggest that erythroid progenitors may arise from different levels of the hematopoietic tree. Moreover, the identification of cell surface marker patterns in human BFU-E and CFU-E enhance our ability to perform downstream functional and molecular analyses at the population and single cell level. Advances in these techniques have already revealed novel subpopulations with increased self-renewing capacity, roles for erythroid progenitors in globin gene expression, and insights into pharmacologic mechanisms of glucocorticoids and pomalidomide. Summary Immunophenotypic and molecular characterization resolves the diversity of erythroid progenitors and may ultimately lead to the ability to target these progenitors to ameliorate diseases of dyserythropoiesis.

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Adult human megakaryocyte-erythroid progenitors are in the CD34+CD38mid fraction

Cited by 55 publications

References 40 publications

Clonal analysis of lineage fate in native haematopoiesis

Clonal analysis of lineage fate in native haematopoiesis

Concise Review: Bipotent Megakaryocytic-Erythroid Progenitors: Concepts and Controversies

Characterization, regulation, and targeting of erythroid progenitors in normal and disordered human erythropoiesis

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