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Activation of human CD4+ cells with CD3 and CD46 induces a T-regulatory cell 1 phenotype

Author

Listed:
  • Claudia Kemper

    (Washington University School of Medicine)

  • Andrew C. Chan

    (Genentech, Inc.)

  • Jonathan M. Green

    (Washington University School of Medicine)

  • Kelly A. Brett

    (Washington University School of Medicine
    Washington University School of Medicine)

  • Kenneth M. Murphy

    (Washington University School of Medicine, and Howard Hughes Medical Institute)

  • John P. Atkinson

    (Washington University School of Medicine
    School of Medicine)

Abstract

The immune system must distinguish not only between self and non-self, but also between innocuous and pathological foreign antigens to prevent unnecessary or self-destructive immune responses. Unresponsiveness to harmless antigens is established through central and peripheral processes1. Whereas clonal deletion and anergy are mechanisms of peripheral tolerance2,3, active suppression by T-regulatory 1 (Tr1) cells has emerged as an essential factor in the control of autoreactive cells4. Tr1 cells are CD4+ T lymphocytes that are defined by their production of interleukin 10 (IL-10)5 and suppression of T-helper cells6; however, the physiological conditions underlying Tr1 differentiation are unknown. Here we show that co-engagement of CD3 and the complement regulator CD46 in the presence of IL-2 induces a Tr1-specific cytokine phenotype in human CD4+ T cells. These CD3/CD46-stimulated IL-10-producing CD4+ cells proliferate strongly, suppress activation of bystander T cells and acquire a memory phenotype. Our findings identify an endogenous receptor-mediated event that drives Tr1 differentiation and suggest that the complement system has a previously unappreciated role in T-cell-mediated immunity and tolerance.

Suggested Citation

  • Claudia Kemper & Andrew C. Chan & Jonathan M. Green & Kelly A. Brett & Kenneth M. Murphy & John P. Atkinson, 2003. "Activation of human CD4+ cells with CD3 and CD46 induces a T-regulatory cell 1 phenotype," Nature, Nature, vol. 421(6921), pages 388-392, January.
  • Handle: RePEc:nat:nature:v:421:y:2003:i:6921:d:10.1038_nature01315
    DOI: 10.1038/nature01315
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