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Disruption of a New Forkhead/winged-helix Protein, Scurfin, Results in the Fatal Lymphoproliferative Disorder of the Scurfy Mouse

Overview
Journal Nat Genet
Specialty Genetics
Date 2001 Jan 4
PMID 11138001
Citations 1076
Authors
M E Brunkow
E W Jeffery
K A Hjerrild
B Paeper
L B Clark
S A Yasayko
J E Wilkinson
D Galas
S F Ziegler
F Ramsdell
Affiliations
Soon will be listed here.
Abstract

Scurfy (sf) is an X-linked recessive mouse mutant resulting in lethality in hemizygous males 16-25 days after birth, and is characterized by overproliferation of CD4+CD8- T lymphocytes, extensive multiorgan infiltration and elevation of numerous cytokines. Similar to animals that lack expression of either Ctla-4 or Tgf-beta, the pathology observed in sf mice seems to result from an inability to properly regulate CD4+CD8- T-cell activity. Here we identify the gene defective in sf mice by combining high-resolution genetic and physical mapping with large-scale sequence analysis. The protein encoded by this gene (designated Foxp3) is a new member of the forkhead/winged-helix family of transcriptional regulators and is highly conserved in humans. In sf mice, a frameshift mutation results in a product lacking the forkhead domain. Genetic complementation demonstrates that the protein product of Foxp3, scurfin, is essential for normal immune homeostasis.

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