| Literature DB >> 17218989 |
Stephanie Humblet-Baron1, Blythe Sather, Stephanie Anover, Shirly Becker-Herman, Debora J Kasprowicz, Socheath Khim, Thuc Nguyen, Kelly Hudkins-Loya, Charles E Alpers, Steve F Ziegler, Hans Ochs, Troy Torgerson, Daniel J Campbell, David J Rawlings.
Abstract
Wiskott-Aldrich syndrome protein (WASp) is essential for optimal T cell activation. Patients with WAS exhibit both immunodeficiency and a marked susceptibility to systemic autoimmunity. We investigated whether alterations in Treg function might explain these paradoxical observations. While WASp-deficient (WASp(-/-)) mice exhibited normal thymic Treg generation, the competitive fitness of peripheral Tregs was severely compromised. The total percentage of forkhead box P3-positive (Foxp3(+)) Tregs among CD4(+) T cells was reduced, and WASp(-/-) Tregs were rapidly outcompeted by WASp(+) Tregs in vivo. These findings correlated with reduced expression of markers associated with self-antigen-driven peripheral Treg activation and homing to inflamed tissue. Consistent with these findings, WASp(-/-) Tregs showed a reduced ability to control aberrant T cell activation and autoimmune pathology in Foxp3(-/-)Scurfy (sf) mice. Finally, WASp(+) Tregs exhibited a marked selective advantage in vivo in a WAS patient with a spontaneous revertant mutation, indicating that altered Treg fitness likely explains the autoimmune features in human WAS.Entities:
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Year: 2007 PMID: 17218989 PMCID: PMC1764857 DOI: 10.1172/JCI29539
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808