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Langerhans cells are generated by two distinct PU.1-dependent transcriptional networks.


ABSTRACT: Langerhans cells (LCs) are the unique dendritic cells found in the epidermis. While a great deal of attention has focused on defining the developmental origins of LCs, reports addressing the transcriptional network ruling their differentiation remain sparse. We addressed the function of a group of key DC transcription factors-PU.1, ID2, IRF4, and IRF8-in the establishment of the LC network. We show that although steady-state LC homeostasis depends on PU.1 and ID2, the latter is dispensable for bone marrow-derived LCs. PU.1 controls LC differentiation by regulating the expression of the critical TGF-? responsive transcription factor RUNX3. PU.1 directly binds to the Runx3 regulatory elements in a TGF-?-dependent manner, whereas ectopic expression of RUNX3 rescued LC differentiation in the absence of PU.1 and promoted LC differentiation from PU.1-sufficient progenitors. These findings highlight the dual molecular network underlying LC differentiation, and show the central role of PU.1 in these processes.

SUBMITTER: Chopin M 

PROVIDER: S-EPMC3865480 | biostudies-literature | 2013 Dec

REPOSITORIES: biostudies-literature

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Langerhans cells are generated by two distinct PU.1-dependent transcriptional networks.

Chopin Michaël M   Seillet Cyril C   Chevrier Stéphane S   Wu Li L   Wang Hongsheng H   Morse Herbert C HC   Belz Gabrielle T GT   Nutt Stephen L SL  

The Journal of experimental medicine 20131118 13


Langerhans cells (LCs) are the unique dendritic cells found in the epidermis. While a great deal of attention has focused on defining the developmental origins of LCs, reports addressing the transcriptional network ruling their differentiation remain sparse. We addressed the function of a group of key DC transcription factors-PU.1, ID2, IRF4, and IRF8-in the establishment of the LC network. We show that although steady-state LC homeostasis depends on PU.1 and ID2, the latter is dispensable for b  ...[more]

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