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Batf3 selectively determines acquisition of CD8+ dendritic cell phenotype and function.

ABSTRACT: Batf3 is a transcription factor that impacts the development of CD103+ tissue-resident dendritic cells (DCs). However, whether Batf3 is absolutely required for the development of CD8+ DCs remains controversial. Id2 is required for CD8+ DC development. Here we show that bone marrow chimeric mice with a deletion of Id2 in the CD11c compartment lose the ability to reject a skin graft expressing a non-self protein antigen or mount a delayed hypersensitivity response. In contrast, Batf3-/- mice remained competent for skin graft rejection and delayed hypersensitivity, and retained a CD8+ DC population with markers characteristic of the CD11b+ DC lineage, including CD11b, CD4 and CD172?, as well as the key regulator transcription factor IRF4, but lacked IRF8 expression. CD8+ DCs in Batf3-/- mice took up and cleaved protein antigen and larger particles but were unable to phagocytose dying cells, a characteristic feature to the CD8+ DC lineage. These data clarify a requirement for CD8+ lineage DCs to induce effectors of neo-antigen-driven skin graft rejection, and improve our understanding of DC subtype commitment by demonstrating that in the absence of Batf3 CD8+ DCs can change their fate and become CD11b+ DCs.

SUBMITTER: Chandra J 

PROVIDER: S-EPMC5309136 | biostudies-literature | 2017 Feb

REPOSITORIES: biostudies-literature

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Batf3 selectively determines acquisition of CD8<sup>+</sup> dendritic cell phenotype and function.

Chandra Janin J   Kuo Paula T Y PT   Hahn Anne M AM   Belz Gabrielle T GT   Frazer Ian H IH  

Immunology and cell biology 20161129 2

Batf3 is a transcription factor that impacts the development of CD103<sup>+</sup> tissue-resident dendritic cells (DCs). However, whether Batf3 is absolutely required for the development of CD8<sup>+</sup> DCs remains controversial. Id2 is required for CD8<sup>+</sup> DC development. Here we show that bone marrow chimeric mice with a deletion of Id2 in the CD11c compartment lose the ability to reject a skin graft expressing a non-self protein antigen or mount a delayed hypersensitivity response.  ...[more]

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