Direct Expansion of Functional CD25+ CD4+ Regulatory T Cells by Antigen-processing Dendritic Cells

Yamazaki, Sayuri; Iyoda, Tomonori; Tarbell, Kristin V.; Olson, Kara; Velinzon, Klara; Inaba, Kayo; Steinman, Ralph M.

doi:10.1084/jem.20030422

articleThe Journal of Experimental MedicineJul 21, 2003BRONZE OA

Direct Expansion of Functional CD25+ CD4+ Regulatory T Cells by Antigen-processing Dendritic Cells

SYSayuri Yamazaki TITomonori Iyoda KVKristin V. Tarbell KOKara Olson KVKlara Velinzon

Rockefeller University · Kyoto University

PubMed

Indexed incrossrefpubmed

Abstract

An important pathway for immune tolerance is provided by thymic-derived CD25+ CD4+ T cells that suppress other CD25- autoimmune disease-inducing T cells. The antigen-presenting cell (APC) requirements for the control of CD25+ CD4+ suppressor T cells remain to be identified, hampering their study in experimental and clinical situations. CD25+ CD4+ T cells are classically anergic, unable to proliferate in response to mitogenic antibodies to the T cell receptor complex. We now find that CD25+ CD4+ T cells can proliferate in the absence of added cytokines in culture and in vivo when stimulated by antigen-loaded dendritic cells (DCs), especially mature DCs. With high doses of DCs in culture, CD25+ CD4+ and CD25-…

Citation impact

858

total citations

FWCI: 27.96
Percentile: 100%
References: 55

Citations per year

Authors

7

Topics & keywords

Topics

Keywords

IL-2 receptor
Interleukin 21
Antigen-presenting cell
Biology
Antigen
T cell
Cell biology
Natural killer T cell

UN Sustainable Development Goals

Good health and well-being

No related works found for this paper.

Funding

NI
National Institutes of Health