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PMID: 17371969
UKPMCID: 17371969

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Incomplete depletion and rapid regeneration of Foxp3+ regulatory T cells following anti-CD25 treatment in malaria-infected mice.

Couper, Kevin N; Blount, Daniel G; de Souza, J Brian; Suffia, Isabelle; Belkaid, Yasmine; Riley, Eleanor M

Journal of immunology (Baltimore, Md. : 1950). 2007;178(7):4136-46.

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Full-text held externally

PMID: 17371969
UKPMCID: 17371969

Abstract

Investigation of the role of regulatory T cells (Treg) in model systems is facilitated by their depletion using anti-CD25 Abs, but there has been considerable debate about the effectiveness of this strategy. In this study, we have compared the depletion and repopulation of CD4+CD25+Foxp3+ Treg in uninfected and malaria-infected mice using 7D4 and/or PC61 anti-CD25 Abs. We find that numbers and percentages of CD25(high) cells, but not Foxp3+ cells, are transiently reduced after 7D4 treatment, whereas treatment with PC61 alone or in combination with 7D4 (7D4 plus PC61) reduces but does not eliminate Foxp3+ cells for up to 2 wk. Importantly, all protocols fail to eliminate significant populations of CD25-Foxp3+ or CD25(low)Foxp3+ cells, which retain potent regulatory capacity. By adoptive transfer we show that repopulation of the spleen by CD25(high)Foxp3+ cells results from the re-expression of CD25 on peripheral populations of CD25-Foxp3+ but not from the conversion of peripheral Foxp3-) cells. CD25(high)Foxp3+ repopulation occurs more rapidly in 7D4-treated mice than in 7D4 plus PC61-treated mice, reflecting ongoing clearance of emergent CD25+Foxp3+ cells by persistent PC61 Ab. However, in 7D4 plus PC61-treated mice undergoing acute malaria infection, repopulation of the spleen by CD25+Foxp3+ cells occurs extremely rapidly, with malaria infection driving proliferation and CD25 expression in peripheral CD4+CD25-Foxp3+ cells and/or conversion of CD4+CD25-Foxp3- cells. Finally, we reveal an essential role for IL-2 for the re-expression of CD25 by Foxp3+ cells after anti-CD25 treatment and observe that TGF-beta is required, in the absence of CD25 and IL-2, to maintain splenic Foxp3+ cell numbers and a normal ratio of Treg:non-Treg cells.

Bibliographic metadata

Type of resource:

text

Content type:

Journal article

Publication type:

Review article

Author(s):

Published date:

2007-04-1

Article title:

Incomplete depletion and rapid regeneration of Foxp3+ regulatory T cells following anti-CD25 treatment in malaria-infected mice.

Journal title:

Journal of immunology (Baltimore, Md. : 1950)

Abbreviated journal title:

J Immunol

ISSN:

0022-1767

Place of publication:

United States

Volume:

178

Issue:

Pagination:

4136-46

Pubmed Identifier:

17371969

Pii Identifier:

178/7/4136

Funder acknowledgement:

Access state:

Active

Institutional metadata

University researcher(s):

Couper, Kevin

Academic department(s):

Faculty of Life Sciences

Record metadata

Manchester eScholar ID:

uk-ac-man-scw:158630

Created by:

Couper, Kevin

Created:

6th April, 2012, 11:18:31

Last modified by:

Couper, Kevin

Last modified:

14th February, 2016, 20:20:42