Lymphoid origin of intrinsically activated plasmacytoid dendritic cells in mice

小鼠体内固有激活的浆细胞样树突状细胞的淋巴来源

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作者:Alessandra Machado Araujo # ,Joseph D Dekker # ,Kendra Garrison ,Zhe Su ,Catherine Rhee ,Zicheng Hu ,Bum-Kyu Lee ,Daniel Osorio ,Jiwon Lee ,Vishwanath R Iyer ,Lauren I R Ehrlich ,George Georgiou ,Gregory Ippolito ,Stephen Yi ,Haley O Tucker

Abstract

We identified a novel mouse plasmacytoid dendritic cell (pDC) lineage derived from the common lymphoid progenitors (CLPs) that is dependent on expression of Bcl11a. These CLP-derived pDCs, which we refer to as 'B-pDCs', have a unique gene expression profile that includes hallmark B cell genes, normally not expressed in conventional pDCs. Despite expressing most classical pDC markers such as SIGLEC-H and PDCA1, B-pDCs lack IFN-α secretion, exhibiting a distinct inflammatory profile. Functionally, B-pDCs induce T cell proliferation more robustly than canonical pDCs following Toll-like receptor 9 (TLR9) engagement. B-pDCs, along with another homogeneous subpopulation of myeloid-derived pDCs, display elevated levels of the cell surface receptor tyrosine kinase AXL, mirroring human AXL+ transitional DCs in function and transcriptional profile. Murine B-pDCs therefore represent a phenotypically and functionally distinct CLP-derived DC lineage specialized in T cell activation and previously not described in mice.

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