Correlation between differentiation plasticity and mRNA expression profiling of CD34+-derived CD14− and CD14+ human normal myeloid precursors

被引:0
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作者
M Montanari
C Gemelli
E Tenedini
T Zanocco Marani
T Vignudelli
M Siena
R Zini
S Salati
G Chiossi
E Tagliafico
R Manfredini
A Grande
S Ferrari
机构
[1] Sezione di Chimica Biologica,Dipartimento di Scienze Biomediche
[2] Università di Modena e Reggio Emilia,Dipartimento di Scienze Ginecologiche
[3] Ostetriche e Pediatriche,undefined
[4] Università di Modena e Reggio Emilia,undefined
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normal myeloid precursors; lineage switching; trans-differentiation;
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摘要
In spite of their apparently restricted differentiation potentiality, hematopoietic precursors are plastic cells able to trans-differentiate from a maturation lineage to another. To better characterize this differentiation plasticity, we purified CD14− and CD14+ myeloid precursors generated by ‘in vitro’ culture of human CD34+ hematopoietic progenitors. Morphological analysis of the investigated cell populations indicated that, as expected, they consisted of granulocyte and monocyte precursors, respectively. Treatment with differentiation inducers revealed that CD14− cells were bipotent granulo-monocyte precursors, while CD14+ cells appeared univocally committed to a terminal macrophage maturation. Flow cytometry analysis demonstrated that the conversion of granulocyte precursors to the mono-macrophage maturation lineage occurs through a differentiation transition in which the granulocyte-related myeloperoxidase enzyme and the monocyte-specific CD14 antigen are co-expressed. Expression profiling evidenced that the observed trans-differentiation process was accompanied by a remarkable upregulation of the monocyte-related MafB transcription factor.
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页码:1588 / 1600
页数:12
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