Existence of CD8α-like dendritic cells with a conserved functional specialization and a common molecular signature in distant mammalian species - PubMed (original) (raw)
Comparative Study
. 2010 Sep 15;185(6):3313-25.
doi: 10.4049/jimmunol.1000824. Epub 2010 Aug 11.
Céline Urien, Rachel Guiton, Yannick Alexandre, Thien-Phong Vu Manh, Thibault Andrieu, Karine Crozat, Luc Jouneau, Nicolas Bertho, Mathieu Epardaud, Jayne Hope, Ariel Savina, Sebastian Amigorena, Michel Bonneau, Marc Dalod, Isabelle Schwartz-Cornil
Affiliations
- PMID: 20702727
- DOI: 10.4049/jimmunol.1000824
Comparative Study
Existence of CD8α-like dendritic cells with a conserved functional specialization and a common molecular signature in distant mammalian species
Vanessa Contreras et al. J Immunol. 2010.
Abstract
The mouse lymphoid organ-resident CD8alpha(+) dendritic cell (DC) subset is specialized in Ag presentation to CD8(+) T cells. Recent evidence shows that mouse nonlymphoid tissue CD103(+) DCs and human blood DC Ag 3(+) DCs share similarities with CD8alpha(+) DCs. We address here whether the organization of DC subsets is conserved across mammals in terms of gene expression signatures, phenotypic characteristics, and functional specialization, independently of the tissue of origin. We study the DC subsets that migrate from the skin in the ovine species that, like all domestic animals, belongs to the Laurasiatheria, a distinct phylogenetic clade from the supraprimates (human/mouse). We demonstrate that the minor sheep CD26(+) skin lymph DC subset shares significant transcriptomic similarities with mouse CD8alpha(+) and human blood DC Ag 3(+) DCs. This allowed the identification of a common set of phenotypic characteristics for CD8alpha-like DCs in the three mammalian species (i.e., SIRP(lo), CADM1(hi), CLEC9A(hi), CD205(hi), XCR1(hi)). Compared to CD26(-) DCs, the sheep CD26(+) DCs show 1) potent stimulation of allogeneic naive CD8(+) T cells with high selective induction of the Ifngamma and Il22 genes; 2) dominant efficacy in activating specific CD8(+) T cells against exogenous soluble Ag; and 3) selective expression of functional pathways associated with high capacity for Ag cross-presentation. Our results unravel a unifying definition of the CD8alpha(+)-like DCs across mammalian species and identify molecular candidates that could be used for the design of vaccines applying to mammals in general.
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