Maternal Alloantigens Promote the Development of Tolerogenic Fetal Regulatory T Cells in Utero

Jeff E. Mold; Jakob Michaëlsson; Trevor D. Burt; Marcus O. Muench; Karen Beckerman; Michael P. Busch; Tzong‐Hae Lee; Douglas F. Nixon; Joseph M. McCune

doi:10.1126/science.1164511

Maternal Alloantigens Promote the Development of Tolerogenic Fetal Regulatory T Cells in Utero

Jeff E. Mold(Karolinska University Hospital), Jakob Michaëlsson(Karolinska University Hospital), Trevor D. Burt(Karolinska University Hospital), Marcus O. Muench(Karolinska University Hospital), Karen Beckerman(Karolinska University Hospital), Michael P. Busch(Karolinska University Hospital), Tzong‐Hae Lee(Karolinska University Hospital), Douglas F. Nixon(Karolinska University Hospital), Joseph M. McCune(Karolinska University Hospital)

Science

December 4, 2008

10.1126/science.1164511

Cited by 827Open Access

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Abstract

As the immune system develops, T cells are selected or regulated to become tolerant of self antigens and reactive against foreign antigens. In mice, the induction of such tolerance is thought to be attributable to the deletion of self-reactive cells. Here, we show that the human fetal immune system takes advantage of an additional mechanism: the generation of regulatory T cells (Tregs) that suppress fetal immune responses. We find that substantial numbers of maternal cells cross the placenta to reside in fetal lymph nodes, inducing the development of CD4+CD25highFoxP3+ Tregs that suppress fetal antimaternal immunity and persist at least until early adulthood. These findings reveal a form of antigen-specific tolerance in humans, induced in utero and probably active in regulating immune responses after birth.

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