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Nature Reviews Immunology
  • Timeline
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FOXP3 and scurfy: how it all began

Nature Reviews Immunologyvolume 14pages343–349 (2014)Cite this article

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Abstract

It has been 65 years since the scurfy mutation arose spontaneously in mice at the Oak Ridge National Laboratory in the United States, and it is 13 years since the molecular cloning of the forkhead box P3(FOXP3) gene was reported. In this Timeline article, we review the events that have occurred during and since this time. This is not meant as an exhaustive review of the biology of FOXP3 or of regulatory T cells, rather it is an attempt to highlight the landmark events that have demonstrated the importance of FOXP3 in immune function. These events have driven, and continue to drive, the extensive research effort to fully understand the role of regulatory T cells in the immune system.

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Figure 1
Figure 2: Structure of the FOXP3 protein.
Figure 3: Conserved non-coding sequences in theFOXP3 gene.

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Acknowledgements

The authors would like to acknowledge W. L. Russell and L. B. Russell for their years of work using genetics to define biological pathways, and V. Godfrey and J. E. Wilkinson for their early characterization of scurfy mice.

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Authors and Affiliations

  1. Novo Nordisk Inflammation Research Center, 530 Fairview Avenue, Seattle, 98109, Washington, USA

    Fred Ramsdell

  2. Benaroya Research Institute, 1201 Ninth Avenue, Seattle, 98101, Washington, USA

    Steven F. Ziegler

Authors
  1. Fred Ramsdell
  2. Steven F. Ziegler

Corresponding author

Correspondence toSteven F. Ziegler.

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The authors declare no competing financial interests.

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