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Selective Expression of the Chemokine Receptor XCR1 on Cross-presenting Dendritic Cells Determines Cooperation with CD8+ T Cells

  • Brigitte G. Dorner
  • Martin B. Dorner
  • Xuefei Zhou
  • Corinna Opitz
  • Ahmed Mora
  • Steffen Güttler
  • Andreas Hutloff
  • Hans W. Mages
  • Katja Ranke
  • Michael Schaefer
  • Robert S. Jack
  • Volker Henn
  • Richard A. Kroczek
Immunity 31(5):p 823-833, November 2009. | DOI: 10.1016/j.immuni.2009.08.027

Summary

The expression of the chemokine receptor XCR1 and the function of its ligand XCL1 (otherwise referred to as ATAC, lymphotactin, or SCM-1) remained elusive to date. In the present report we demonstrated that XCR1 is exclusively expressed on murine CD8+ dendritic cells (DCs) and showed that XCL1 is a potent and highly specific chemoattractant for this DC subset. CD8+ T cells abundantly secreted XCL1 8–36 hr after antigen recognition on CD8+ DCs in vivo, in a period in which stable T cell-DC interactions are known to occur. Functionally, XCL1 increased the pool of antigen-specific CD8+ T cells and their capacity to secrete IFN-γ. Absence of XCL1 impaired the development of cytotoxicity to antigens cross-presented by CD8+ DCs. The XCL1-XCR1 axis thus emerges as an integral component in the development of efficient cytotoxic immunity in vivo.

Copyright © 2009Elsevier, Inc.

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