Haematopoietic stem cell reprogramming and the hope for a universal blood product

doi:10.1002/1873-3468.13681

Review

. 2019 Dec;593(23):3253-3265.

doi: 10.1002/1873-3468.13681. Epub 2019 Dec 2.

Haematopoietic stem cell reprogramming and the hope for a universal blood product

José Gabriel Barcia Durán¹, Raphaël Lis^{1

2}, Shahin Rafii¹

Affiliations

¹ Division of Regenerative Medicine, Department of Medicine, Ansary Stem Cell Institute, Weill Cornell Medicine, New York, NY, USA.
² Ronald O. Perelman and Claudia Cohen Center for Reproductive Medicine and Infertility, Weill Cornell Medicine, New York, NY, USA.

PMID: 31725897
DOI: 10.1002/1873-3468.13681

Free article

Review

Haematopoietic stem cell reprogramming and the hope for a universal blood product

José Gabriel Barcia Durán et al. FEBS Lett. 2019 Dec.

Free article

. 2019 Dec;593(23):3253-3265.

doi: 10.1002/1873-3468.13681. Epub 2019 Dec 2.

Authors

José Gabriel Barcia Durán¹, Raphaël Lis^{1

2}, Shahin Rafii¹

Affiliations

¹ Division of Regenerative Medicine, Department of Medicine, Ansary Stem Cell Institute, Weill Cornell Medicine, New York, NY, USA.
² Ronald O. Perelman and Claudia Cohen Center for Reproductive Medicine and Infertility, Weill Cornell Medicine, New York, NY, USA.

PMID: 31725897
DOI: 10.1002/1873-3468.13681

Abstract

Haematopoietic stem cells (HSCs) are the only adult stem cells with a demonstrated clinical use, even though a tractable method to maintain and expand human HSCs in vitro has not yet been found. Owing to the introduction of transplantation strategies for the treatment of haematological malignancies and, more recently, the promise of gene therapy, the need to improve the generation, manipulation and scalability of autologous or allogeneic HSCs has risen steeply over the past decade. In that context, reprogramming strategies based on the expression of exogenous transcription factors have emerged as a means to produce functional HSCs in vitro. These approaches largely stem from the assumption that key master transcription factors direct the expression of downstream target genes thereby triggering haematopoiesis. Both somatic and pluripotent cells have been used to this end, yielding variable results in terms of haematopoietic phenotype and functionality. Here, we present an overview of the haematopoietic reprogramming methods reported to date, provide the appropriate historical context and offer some critical insight about where the field stands at present.

Keywords: haematopoietic stem cells; pluripotent cell reprogramming; somatic cell reprogramming.

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References

1. Schneuwly S, Klemenz R and Gehring WJ (1987) Redesigning the body plan of Drosophila by ectopic expression of the homoeotic gene Antennapedia. Nature 325, 816-818.
1. Weintraub H, Tapscott SJ, Davis RL, Thayer MJ, Adam MA, Lassar AB and Miller AD (1989) Activation of muscle-specific genes in pigment, nerve, fat, liver, and fibroblast cell lines by forced expression of MyoD (muscle regulatory gene/MyoD retrovirus). Dev Biol 86, 5434-5438.
1. Kulessa H, Frampton J and Graf T (1995) GATA-1 reprograms avian myelomonocytic cell lines into eosinophils, thromboblasts, and erythroblasts. Genes Dev 9, 1250-1262.
1. Nerlov C and Graf T (1998) PU.1 induces myeloid lineage commitment in multipotent hematopoietic progenitors. Genes Dev 12, 2403-2412.
1. Xie H, Ye M, Feng R, Graf T and York N (2004) Stepwise reprogramming of B cells into macrophages. Cell 117, 663-676.

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[1] Schneuwly S, Klemenz R and Gehring WJ (1987) Redesigning the body plan of Drosophila by ectopic expression of the homoeotic gene Antennapedia. Nature 325, 816-818.

[2] Schneuwly S, Klemenz R and Gehring WJ (1987) Redesigning the body plan of Drosophila by ectopic expression of the homoeotic gene Antennapedia. Nature 325, 816-818.

[3] Weintraub H, Tapscott SJ, Davis RL, Thayer MJ, Adam MA, Lassar AB and Miller AD (1989) Activation of muscle-specific genes in pigment, nerve, fat, liver, and fibroblast cell lines by forced expression of MyoD (muscle regulatory gene/MyoD retrovirus). Dev Biol 86, 5434-5438.

[4] Weintraub H, Tapscott SJ, Davis RL, Thayer MJ, Adam MA, Lassar AB and Miller AD (1989) Activation of muscle-specific genes in pigment, nerve, fat, liver, and fibroblast cell lines by forced expression of MyoD (muscle regulatory gene/MyoD retrovirus). Dev Biol 86, 5434-5438.

[5] Kulessa H, Frampton J and Graf T (1995) GATA-1 reprograms avian myelomonocytic cell lines into eosinophils, thromboblasts, and erythroblasts. Genes Dev 9, 1250-1262.

[6] Kulessa H, Frampton J and Graf T (1995) GATA-1 reprograms avian myelomonocytic cell lines into eosinophils, thromboblasts, and erythroblasts. Genes Dev 9, 1250-1262.

[7] Nerlov C and Graf T (1998) PU.1 induces myeloid lineage commitment in multipotent hematopoietic progenitors. Genes Dev 12, 2403-2412.

[8] Nerlov C and Graf T (1998) PU.1 induces myeloid lineage commitment in multipotent hematopoietic progenitors. Genes Dev 12, 2403-2412.

[9] Xie H, Ye M, Feng R, Graf T and York N (2004) Stepwise reprogramming of B cells into macrophages. Cell 117, 663-676.

[10] Xie H, Ye M, Feng R, Graf T and York N (2004) Stepwise reprogramming of B cells into macrophages. Cell 117, 663-676.

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Haematopoietic stem cell reprogramming and the hope for a universal blood product

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Haematopoietic stem cell reprogramming and the hope for a universal blood product

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