Pregnancy induces a fetal antigen-specific maternal T regulatory cell response that contributes to tolerance
- Creators
- Kahn, Daniel A.
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Baltimore, David
Abstract
A fetus is inherently antigenic to its mother and yet is not rejected. The T regulatory (Treg) subset of CD4^+ T cells can limit immune responses and has been implicated in maternal tolerance of the fetus. Using virgin inbred mice undergoing a first syngenic pregnancy, in which only the male fetuses are antigenic, we demonstrate a maternal splenocyte proliferative response to the CD4^+ T cell restricted epitope of the male antigen (H-Y) in proportion to the fetal antigen load. A portion of the maternal immune response to fetal antigens is Treg in nature. The bystander suppressive function of pregnancy-generated Tregs requires the presence of the fetal antigen, demonstrating their inherent antigen specificity. In vivo targeting of diphtheria toxin to kill Tregs leads to a lower fraction of live male offspring and a selective reduction in mass of the surviving males. Thus, Tregs generated in the context of pregnancy function in an antigen-specific manner to limit the maternal immune response to the fetus in a successful pregnancy.
Additional Information
© 2010 by the National Academy of Sciences. Contributed by David Baltimore, March 31, 2010 (sent for review January 22, 2010). Published online before print May 3, 2010. We thank L. Sandoval of the Caltech Office of Laboratory Animal Resources for expert assistance with the timed matings. This work was supported in part by a research grant from the Skirball Foundation (to D.B.). D.A.K. is supported by the National Institutes of Health—Building Interdisciplinary Research Careers in Women's Health (BIRCWH) center at the University of California, Los Angeles (K12 HD001400). Author contributions: D.A.K. and D.B. designed research; D.A.K. performed research; D.A.K. and D.B. analyzed data; and D.K. and D.B. wrote the paper.Attached Files
Published - Kahn2010p10181P_Natl_Acad_Sci_Usa.pdf
Supplemental Material - pnas.201003909SI.pdf
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Additional details
- PMCID
- PMC2889122
- Eprint ID
- 18595
- Resolver ID
- CaltechAUTHORS:20100608-075607749
- Skirball Foundation
- NIH
- K12 HD001400
- Created
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2010-06-13Created from EPrint's datestamp field
- Updated
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2021-11-08Created from EPrint's last_modified field