Characterization of human DNGR-1+ BDCA3+ leukocytes as putative equivalents of mouse CD8α+ dendritic cells

被引:537
作者
Franz Poulin, Lionel [1 ]
Salio, Mariolina [4 ]
Griessinger, Emmanuel [2 ]
Anjos-Afonso, Fernando [2 ]
Craciun, Ligia [5 ]
Chen, Ji-Li [4 ]
Keller, Anna M. [1 ]
Joffre, Olivier [1 ]
Zelenay, Santiago [1 ]
Nye, Emma [3 ]
Le Moine, Alain [5 ]
Faure, Florence [6 ,7 ]
Donckier, Vincent [5 ]
Sancho, David [8 ]
Cerundolo, Vincenzo [4 ]
Bonnet, Dominique [2 ]
Reis e Sousa, Caetano [1 ]
机构
[1] Canc Res UK, London Res Inst, Immunobiol Lab, London WC2A 3PX, England
[2] Canc Res UK, London Res Inst, Haematopoiet Stem Cell Lab, London WC2A 3PX, England
[3] Canc Res UK, London Res Inst, Expt Pathol Labs, London WC2A 3PX, England
[4] Weatherall Inst Mol Med, Nuffield Dept Clin Med, Oxford OX3 9DS, England
[5] Univ Libre Bruxelles, Inst Med Immunol, B-6041 Gosselies, Belgium
[6] INSERM, U932, Paris, France
[7] Inst Curie, Ctr Rech, F-75248 Paris, France
[8] CNIC Spanish Natl Ctr Cardiovasc Res Carlos III, Dept Vasc Biol & Inflammat, Madrid 28029, Spain
关键词
C-TYPE LECTIN; MONOCLONAL-ANTIBODY NLDC-145; SUBSETS IN-VIVO; CROSS-PRESENTATION; TISSUE DISTRIBUTION; LANGERHANS CELLS; DEC-205; PROTEIN; EXPRESSION; ANTIGEN; IDENTIFICATION;
D O I
10.1084/jem.20092618
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
In mouse, a subset of dendritic cells (DCs) known as CD8 alpha(+) DCs has emerged as an important player in the regulation of T cell responses and a promising target in vaccination strategies. However, translation into clinical protocols has been hampered by the failure to identify CD8 alpha(+) DCs in humans. Here, we characterize a population of human DCs that expresses DNGR-1 (CLEC9A) and high levels of BDCA3 and resembles mouse CD8 alpha(+) DCs in phenotype and function. We describe the presence of such cells in the spleens of humans and humanized mice and report on a protocol to generate them in vitro. Like mouse CD8 alpha(+) DCs, human DNGR-1(+) BDCA3(hi) DCs express Necl2, CD207, BATF3, IRF8, and TLR3, but not CD11b, IRF4, TLR7, or (unlike CD8 alpha(+) DCs) TLR9. DNGR-1(+) BDCA3(hi) DCs respond to poly I:C and agonists of TLR8, but not of TLR7, and produce interleukin (IL)-12 when given innate and T cell-derived signals. Notably, DNGR-1(+) BDCA3(+) DCs from in vitro cultures efficiently internalize material from dead cells and can cross-present exogenous antigens to CD8(+) T cells upon treatment with poly I:C. The characterization of human DNGR-1(+) BDCA3(hi) DCs and the ability to grow them in vitro opens the door for exploiting this subset in immunotherapy.
引用
收藏
页码:1261 / 1271
页数:11
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