Cell Reports (Aug 2016)

Differential Intrasplenic Migration of Dendritic Cell Subsets Tailors Adaptive Immunity

  • Samuele Calabro,
  • Dong Liu,
  • Antonia Gallman,
  • Manuela Sales L. Nascimento,
  • Zizi Yu,
  • Ting-ting Zhang,
  • Pei Chen,
  • Biyan Zhang,
  • Lan Xu,
  • Uthaman Gowthaman,
  • Jayendra Kumar Krishnaswamy,
  • Ann M. Haberman,
  • Adam Williams,
  • Stephanie C. Eisenbarth

DOI
https://doi.org/10.1016/j.celrep.2016.07.076
Journal volume & issue
Vol. 16, no. 9
pp. 2472 – 2485

Abstract

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Evidence suggests that distinct splenic dendritic cell (DC) subsets activate either CD4+ or CD8+ T cells in vivo. This bias has been partially ascribed to differential antigen presentation; however, all DC subsets can activate both T cell lineages in vitro. Therefore, we tested whether the organization of DC and T cell subsets in the spleen dictated this preference. We discovered that CD4+ and CD8+ T cells segregated within splenic T cell zones prior to immunization. After intravenous immunization, the two major conventional DC populations, distinguished by 33D1 and XCR1 staining, migrated into separate regions of the T cell zone: 33D1+ DCs migrated into the CD4+ T cell area, whereas XCR1+ DCs migrated into the CD8+ T cell area. Thus, the post-immunization location of each DC subset correlated with the T cell lineage it preferentially primes. Preventing this co-localization selectively impaired either CD4+ or CD8+ T cell immunity to blood-borne antigens.

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