Thiol-mediated Redox Regulation of Intestinal Lamina Propria T

doi:10.1084/jem.192.6.907

Published online 18 September 2000.

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© The Rockefeller University Press, 0022-1007/2000/9/907/ $5.00
The Journal of Experimental Medicine, Volume 192, Number 6, September 18, 2000 907-912

Brief Definitive Reports

Thiol-mediated Redox Regulation of Intestinal Lamina Propria T Lymphocytes

Bernd Sido^a, Jutta Braunstein^b, Raoul Breitkreutz^c, Christian Herfarth^a, and Stefan C. Meuer^b
^a Department of Surgery, University of Heidelberg, 69120 Heidelberg, Germany
^b Institute of Immunology, University of Heidelberg, 69120 Heidelberg, Germany
^c German Cancer Research Center, 69120 Heidelberg, Germany

Correspondence to: Stefan C. Meuer, Institute of Immunology, University of Heidelberg, Im Neuenheimer Feld 305, 69120 Heidelberg, Germany. Tel:49-6221-56-4000 Fax:49-6221-56-5990

Intestinal lamina propria T lymphocytes (LP-Ts) have a markedlylow proliferative potential both in vivo and in vitro. Here,we have identified that the capacity of antigen-presenting cellsto release cysteine upon receptor–ligand interactionsrepresents a critical parameter for proliferation of LP-Ts.The availability of cysteine is limiting for the intracellularproduction of glutathione, which in turn is essential for cellcycle progression. When cysteine is provided either directlyor by addition of the reducing agent 2-mercaptoethanol to cystine-containingculture medium, proliferation of LP-T is fully restored. Importantly,coculture with peripheral blood monocytes that easily take upcystine, reduce cystine, and secrete cysteine also restoresreactivity of LP-Ts to T cell receptor/CD3 stimulation. In markedcontrast, lamina propria macrophages lack this capacity to elaboratecysteine, and thereby secure physiological unresponsivenessto antigen exposure in the intestinal microenvironment. Thewell-documented local recruitment of blood monocytes in inflammatorybowel disease (IBD) may thus represent an important parameterunderlying hyperresponsiveness of T cells, an essential componentof the pathogenesis of IBD.

Key Words: macrophage, monocyte, inflammatory bowel disease, cysteine,glutathione

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