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MiR144/451 Expression Is Repressed by RUNX1 During Megakaryopoiesis and Disturbed by RUNX1/ETO
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نویسنده
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kohrs n. ,kolodziej s. ,kuvardina o.n. ,herglotz j. ,yillah j. ,herkt s. ,piechatzek a. ,salinas riester g. ,lingner t. ,wichmann c. ,bonig h. ,seifried e. ,platzbecker u. ,medyouf h. ,grez m. ,lausen j.
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منبع
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plos genetics - 2016 - دوره : 12 - شماره : 3
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چکیده
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A network of lineage-specific transcription factors and micrornas tightly regulates differentiation of hematopoietic stem cells along the distinct lineages. deregulation of this regulatory network contributes to impaired lineage fidelity and leukemogenesis. we found that the hematopoietic master regulator runx1 controls the expression of certain micrornas,of importance during erythroid/megakaryocytic differentiation. in particular,we show that the erythorid mir144/451 cluster is epigenetically repressed by runx1 during megakaryopoiesis. furthermore,the leukemogenic runx1/eto fusion protein transcriptionally represses the mir144/451 pre-microrna. thus runx1/eto contributes to increased expression of mir451 target genes and interferes with normal gene expression during differentiation. furthermore,we observed that inhibition of runx1/eto in kasumi1 cells and in runx1/eto positive primary acute myeloid leukemia patient samples leads to up-regulation of mir144/451. runx1 thus emerges as a key regulator of a microrna network,driving differentiation at the megakaryocytic/erythroid branching point. the network is disturbed by the leukemogenic runx1/eto fusion product. © 2016 kohrs et al.
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آدرس
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georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, heinrich-pette-institute,leibniz institute for experimental virology,hamburg, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, medical-university goettingen,transcriptome analysis laboratory,goettingen, Germany, medical-university goettingen,transcriptome analysis laboratory,goettingen, Germany, department of transfusion medicine,cell therapeutics and hemostaseology,ludwig-maximilian university hospital,munich, Germany, institute for transfusion medicine and immunohematology,johann-wolfgang-goethe university and german red cross blood service,frankfurt am main, Germany, institute for transfusion medicine and immunohematology,johann-wolfgang-goethe university and german red cross blood service,frankfurt am main, Germany, department of hematology,medical clinic and polyclinic i,university hospital carl gustav carus,dresden, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt, Germany, georg-speyer-haus,institute for tumorbiology and experimental therapy,frankfurt,germany,institute for transfusion medicine and immunohematology,johann-wolfgang-goethe university and german red cross blood service,frankfurt am main, Germany
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Authors
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