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MicroRNA-708 is a novel regulator of the Hoxa9 program in myeloid cells
by
Sperb Nadine
, Humphries, Keith
, Delsing, Malmberg Erik
, Döhner Hartmut
, Kumar, Kopparapu Pradeep
, Larsson, Erik
, Pochert Nicole
, Wiese, Sebastian
, Xiang Ping
, Iben, Sebastian
, Hirst, Martin
, Miller, Christina
, Lorzadeh Alireza
, Ruess Christoph
, Krowiorz Kathrin
, Fogelstrand Linda
, Kanduri Meena
, Döhner Konstanze
, Rouhi Arefeh
, Grasedieck Sarah
, Rösler Reinhild
, MacPhee, Liam
, Ashouri Arghavan
, Kuchenbauer Florian
, Escano Leo
, Heravi-Moussavi Alireza
, Staffas, Anna
, Schneider, Edith
, Palmqvist Lars
in
Acute myeloid leukemia
/ Cell death
/ Cell differentiation
/ Cell self-renewal
/ CRISPR
/ Deregulation
/ Epigenetics
/ Gene expression
/ Gene regulation
/ Genes
/ Genetic transformation
/ Hematopoiesis
/ Homeobox
/ HOX gene
/ Leukemia
/ Leukemogenesis
/ MicroRNAs
/ miRNA
/ Modulation
/ Myeloid cells
/ Myeloid leukemia
/ Phenotypes
/ Transcription
/ Tumor suppressor genes
2020
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MicroRNA-708 is a novel regulator of the Hoxa9 program in myeloid cells
by
Sperb Nadine
, Humphries, Keith
, Delsing, Malmberg Erik
, Döhner Hartmut
, Kumar, Kopparapu Pradeep
, Larsson, Erik
, Pochert Nicole
, Wiese, Sebastian
, Xiang Ping
, Iben, Sebastian
, Hirst, Martin
, Miller, Christina
, Lorzadeh Alireza
, Ruess Christoph
, Krowiorz Kathrin
, Fogelstrand Linda
, Kanduri Meena
, Döhner Konstanze
, Rouhi Arefeh
, Grasedieck Sarah
, Rösler Reinhild
, MacPhee, Liam
, Ashouri Arghavan
, Kuchenbauer Florian
, Escano Leo
, Heravi-Moussavi Alireza
, Staffas, Anna
, Schneider, Edith
, Palmqvist Lars
in
Acute myeloid leukemia
/ Cell death
/ Cell differentiation
/ Cell self-renewal
/ CRISPR
/ Deregulation
/ Epigenetics
/ Gene expression
/ Gene regulation
/ Genes
/ Genetic transformation
/ Hematopoiesis
/ Homeobox
/ HOX gene
/ Leukemia
/ Leukemogenesis
/ MicroRNAs
/ miRNA
/ Modulation
/ Myeloid cells
/ Myeloid leukemia
/ Phenotypes
/ Transcription
/ Tumor suppressor genes
2020
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MicroRNA-708 is a novel regulator of the Hoxa9 program in myeloid cells
by
Sperb Nadine
, Humphries, Keith
, Delsing, Malmberg Erik
, Döhner Hartmut
, Kumar, Kopparapu Pradeep
, Larsson, Erik
, Pochert Nicole
, Wiese, Sebastian
, Xiang Ping
, Iben, Sebastian
, Hirst, Martin
, Miller, Christina
, Lorzadeh Alireza
, Ruess Christoph
, Krowiorz Kathrin
, Fogelstrand Linda
, Kanduri Meena
, Döhner Konstanze
, Rouhi Arefeh
, Grasedieck Sarah
, Rösler Reinhild
, MacPhee, Liam
, Ashouri Arghavan
, Kuchenbauer Florian
, Escano Leo
, Heravi-Moussavi Alireza
, Staffas, Anna
, Schneider, Edith
, Palmqvist Lars
in
Acute myeloid leukemia
/ Cell death
/ Cell differentiation
/ Cell self-renewal
/ CRISPR
/ Deregulation
/ Epigenetics
/ Gene expression
/ Gene regulation
/ Genes
/ Genetic transformation
/ Hematopoiesis
/ Homeobox
/ HOX gene
/ Leukemia
/ Leukemogenesis
/ MicroRNAs
/ miRNA
/ Modulation
/ Myeloid cells
/ Myeloid leukemia
/ Phenotypes
/ Transcription
/ Tumor suppressor genes
2020
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MicroRNA-708 is a novel regulator of the Hoxa9 program in myeloid cells
Journal Article
MicroRNA-708 is a novel regulator of the Hoxa9 program in myeloid cells
2020
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Overview
MicroRNAs (miRNAs) are commonly deregulated in acute myeloid leukemia (AML), affecting critical genes not only through direct targeting, but also through modulation of downstream effectors. Homeobox (Hox) genes balance self-renewal, proliferation, cell death, and differentiation in many tissues and aberrant Hox gene expression can create a predisposition to leukemogenesis in hematopoietic cells. However, possible linkages between the regulatory pathways of Hox genes and miRNAs are not yet fully resolved. We identified miR-708 to be upregulated in Hoxa9/Meis1 AML inducing cell lines as well as in AML patients. We further showed Meis1 directly targeting miR-708 and modulating its expression through epigenetic transcriptional regulation. CRISPR/Cas9 mediated knockout of miR-708 in Hoxa9/Meis1 cells delayed disease onset in vivo, demonstrating for the first time a pro-leukemic contribution of miR-708 in this context. Overexpression of miR-708 however strongly impeded Hoxa9 mediated transformation and homing capacity in vivo through modulation of adhesion factors and induction of myeloid differentiation. Taken together, we reveal miR-708, a putative tumor suppressor miRNA and direct target of Meis1, as a potent antagonist of the Hoxa9 phenotype but an effector of transformation in Hoxa9/Meis1. This unexpected finding highlights the yet unexplored role of miRNAs as indirect regulators of the Hox program during normal and aberrant hematopoiesis.
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